Abstract
Marine organisms often produce a variety of metabolites with unique structures and diverse biological activities that enable them to survive and struggle in the extremely challenging environment. During the last two decades, our group devoted great effort to the discovery of pharmaceutically interesting lead compounds from South China Sea marine plants and invertebrates. We discovered numerous marine secondary metabolites spanning a wide range of structural classes, various biosynthetic origins and various aspects of biological activities. In a series of reviews, we have summarized the bioactive natural products isolated from Chinese marine flora and fauna found during 2000–2012. The present review provides an updated summary covering our latest research progress and development in the last decade (2012–2022) highlighting the discovery of over 400 novel marine secondary metabolites with promising bioactivities from South China Sea marine organisms.
Similar content being viewed by others
Introduction
The ocean supports vast habitats and serves as prolific resources for various living organisms. Given the uniqueness of ocean habitat, high concentration of salts, high pressure, low concentration of oxygen, and dark condition, marine organisms often produce highly potent metabolites with unique structures and diverse biological activities to enable them to survive and struggle in the extremely challenging environments. Since one of the first marine-derived drugs, cytarabine, was approved in 1969 by the U.S. Food and Drug Administration (FDA) for the treatment of leukemia, inspiring more and more scientists to devote great effort to the development of marine drugs [1]. In recent decades, the rapid development of the biotechnology has led to a new era of bioprospecting for marine natural products. The efficiency of drug discovery has been greatly improved as the revolutionary target screening methods were widely applicated. Several marine drugs and drug candidates in preclinical or clinical trials undoubtedly proved that marine natural products are important inspiration sources for drug development.
Located in tropical and subtropical areas, the South China Sea is an important geographic location yielding many novel marine natural products, most likely due to the remarkable biodiversity of coral reefs, which provide a suitable environment for the wide range of marine organisms. As a pioneer in the chemical investigation of Chinese marine organisms, our group, the only group in Shanghai Institute of Materia Medica (SIMM), has long been dedicating on the discovery of pharmaceutically interesting lead compounds from marine plants and invertebrates since 2000. We have continuously reported hundreds of marine compounds with novel structural skeletons from marine sponges, soft corals, marine algae and so on, resulting in numerous publications in reputable journals, and our research results have been serially invited reviews including Chemical Reviews [2, 3], Natural Product Reports [4,5,6], as well as Acta Pharmacologica Sinica [7]. As great recent progress on marine natural products has been achieved by our group, an update of the previous summary was highly urgent. On the occasion of the 90th anniversary of SIMM, we will take this opportunity to showcase the main research progress of our group in the past 10 years. In this review, it covers more than 100 literatures and summarize over 400 novel marine metabolites with interesting biological activities reported by our group since 2012. Some classic cases are described in detail.
Chemical studies on marine plants
Marine plants are primary producers playing important roles in the marine ecosystem. They are autotrophic organisms that use chlorophyll to produce organic nutrient in the ocean. There are many phyla of marine plants, ranging from low eukaryotic algae to higher seed plants. Our group has long been engaged in the chemical investigation of various marine algae and mangroves, because of their nutritional or medicinal values. In this section, it will mainly discuss the chemistry and bioactivity of structurally and biologically interesting metabolites from marine algae and mangrove plants discovered by our group.
Marine algae
Marine algae comprise large number of simple organisms relying on photosynthesis. In general, algae can be classified into two main groups. The first one is the microalgae, which includes blue green algae, dinoflagellates, bacillariophyta, etc. The second group is macroalgae (seaweeds) which includes green, brown, and red algae. Most of our studies involve algae belonging to the phyla Chlorophyta, Phaeophyta, and Rhodophyta. A series of unusual compounds bearing unprecedented structures were identified in these taxa.
Caulerpa racemosa is a species of edible green alga belonging to the phylum Chlorophyta. It is commonly known as sea grapes and is mainly distributed in Guangdong Province, Guangxi Autonomous Region, Dongsha and Xisha Islands in China. C. racemosa is a kind of traditional Chinese medicine, which was first recorded in the Compendium of Xinhua Materia Medica for the treatment of various pains caused by qi stagnation and blood stasis. As part of our continuing studies on the chemical constituents of the C. racemosa, the green algae were collected from the coastline of Zhanjiang city, Guangdong Province, led to the isolation of two bisindole alkaloids, racemosins A (1) and B (2), and one well-known pigment caulerpin (S1) [8] (Fig. 1 and Supplementary Fig. S1). Compound 1 possesses a structurally unique seco-indolo[3,2-a]carbazole skeleton with two uncommon indolinenone units both conjugated with a methyl propenoate moiety, which represents the first example of a bisindole alkaloid with the seco-indolo[3,2-a] carbazole skeleton from nature. Comparing the chemical structures of 1 and 2, it is easy to find that they are biogenetically related to each other with an unusual indolo[3,2-a] carbazole. In a neuro-protective assay, compound 1 significantly attenuated the Aβ25–35-induced SH-SY5Y cell damage with a 14.6% increase in cell viability at the concentration of 10 μM, when compared to epigallocatechin gallate (16.57% increase at 10 μM) as the positive control.
Structures of new isolates from marine algae.
Sargassum thunbergii belongs to the phylum Phaeophyta. As a common economic brown alga in coastal areas of China, S. thunbergii has strong reproductive capacity, which plays an important regulatory role in maintaining the balance of coastal ecosystem. It is well known that marine algae are ideal health food for diabetics. In our chemical and biological studies of the S. thunbergii, which were collected off the coast of Nanji Island, Zhejiang Province, China, resulting in the isolation of a new sterol thunberol (3). The compound exhibited significant inhibitory activity against protein tyrosine phosphatase 1B (PTP1B), a potential drug target for the treatment of type-II diabetes, with the IC50 value of 2.24 μg/mL [9]. This result provided an inspiration for the development of marine algae products in the prevention of diabetes.
Red algae of the genus Laurencia are well-known for their ability to biosynthesize an astonishing variety of structurally unusual secondary metabolites. More than 1100 different metabolites have been characterized from approximately 80 species of this genus. Among them, cuparene-type, and laurane-type sesquiterpenoids are well-known and typical. Two chemical investigations of the red algae L. okamurai Yamada, which were collected off the coast of Nanji Island, Zhejiang Province in 2010 [10] and 2013 [11, 12], led to the isolation of a novel rearranged sesquiterpene seco-laurokamurone (4), six new laurane-type sesquiterpenes (5–10), one new laurokamurane-type sesquiterpene (11), one new bisabolane-type sesquiterpene (12) and three novel heterodimeric laurane-type sesquiterpenoids laurokamurols A–C (13–15) (Fig. 1). The absolute configurations of the new bis-sesquitepenoids (13–15), especially their axial chirality, were determined by extensive spectroscopic analyses and time-dependent density functional theory electronic circular dichroism (TDDFT-ECD) method. In bioassay, laurokamurols A–C (13–15) and the known related compounds showed promising PTP1B inhibitory activities with the IC50 values ranging from 4.9 to 14.9 μg/mL [11, 12]. These biological components of the marine algae suggest the possible utilization as food additives with the functions for human healthcare, especially for anti-diabetic aspect.
Mangroves
Mangroves, mainly distributed in the tropical and subtropical tidelands, are distinct plant communities that have attracted as much curiosity and scientific attention for their salt-tolerant habits. This special ecosystem is usually found in Asia and Australia with diverse species. For example, more than 40% of mangrove forests are found along the Asian coasts, including the South China Sea Coast. In many countries, especially in China, the extracts and chemicals from mangroves are used mainly in folkloric medicine, as insecticides and piscicides and these practices continue to today. The chemical and biological studies of the plants are very important for deciphering the actual value of folkloric remedies.
In the course of our ongoing research for bioactive metabolites from mangrove plants, we investigated the twigs and leaves of Xylocarpus granatum (Meliaceae), collected from the seashore of Dongzhai, Hainan Province, China, resulting in the isolation of four new 8,9,30-phragmalin orthoesters (16–19), along with six related known compounds, namely xyloccensins O–S and V [13]. It is worth mentioning that the absolute configurations of xyloccensins O–S and V were revised via X‑ray diffraction analysis and TDDFT-ECD calculation. Later, 6-O-acetyl xylocarpin D (S2) [14], 1,2-dihydro-3α-hydroxy-turranolide (S3) [14] and xylogranatumines A–G (S4–S8, 20, and S9) [15] were also successively isolated and determined (Fig. 2 and Supplementary Fig. S2). Biogenetically, these interesting molecules might be derived from hainangranatumin D, a limonoid previously isolated from X. granatum. In bioassay, xylogranatumine F (20) exhibited weak cytotoxic activity against A549 tumor cells with inhibition of 54.2% at the concentration of 10 μM.
Structures of representative compounds from mangroves.
Besides, some new tetranortritepenoids (21–23 and S10–S12) (Fig. 2 and Supplementary Fig. S2) were discovered and determined by detailed spectroscopic analysis. Among them, the absolute configuration of 9-epixylogranatin A (22) was determined by TDDFT-ECD calculation. Xylogranatumin A (23) represents the first example of the 9,10-seco limonoid with an unprecedented B ring bearing an oxygen bridge between C-1 and C-8 [14]. Xylogranatopyridines A and B (24 and 25) were two new pyridine-containing limonoids, their structures were elucidated unambiguously by single-crystal X-ray diffraction analysis. In addition, xylogranatopyridine A (24) was found to be the first limonoid to show inhibitory activity against PTP1B with the IC50 value of 22.9 μM [16].
Acanthus ilicifolius Linn. (Acanthaceae), a gregarious shrub, widely distributed in coastal regions of southeastern China. It has long been used as a traditional Chinese medicine for treatment against rheumatism, paralysis, and asthma. Chemical investigation of the leaves and stems of A. ilicifolius Linn., collected at the Zhanjiang mangrove national nature reserve, Guangdong Province, China, led to the isolation of one new pyrido[1,2-a]indole alkaloid acanthiline A (26) (Fig. 2) [17]. A plausible biosynthetic pathway for 26 from tryptophan was proposed as shown in Scheme 1.
Possible biosynthesis of acanthiline A (26) in Acanthus ilicifolius.
Chemical studies on marine invertebrates
Marine invertebrates have been categorized into over 30 phyla. Most marine invertebrates lack physical protection in the form of an exoskeleton, for example, spines, stings, or shells. Therefore, marine organisms developed unique metabolic pathways and, thus, the capability to produce a wide variety of toxic chemicals to mediate spatial competition as well as to prevent parasitism and predation. According to our study, marine sponges, soft corals, and mollusks are the most productive invertebrates contributing numerous biomolecules.
Sponges
Sponges (phylum Porifera) are the most primitive of multicellular animals evolved from about 600 million years ago, and one of the most important reef-building organisms in benthic biomes worldwide. Sponges, which are nerveless and muscleless, are simple in structure but diverse in variety. Over the past decade, a series of chemical investigations of the sponge samples collected from the South China Sea were conducted by our group.
For instance, a new isomalabaricane triterpene, stellettin N (S13) [18], was isolated from the marine sponge Stelletta sp. from Hainan Province. A novel sesquiterpene pyridine alkaloid fasciospyrinadine (S14) [19] was isolated from the sponge Fasciospongia sp. collected from Weizhou Island, Guangxi Autonomous Region. Two new indole alkaloids (S15 and S16) [20], and one new β-carboline alkaloid (S17) [20] were isolated from the Hainan marine sponge Hyrtios erecta (Supplementary Fig. S3).
Sponges of the genus Xestospongia are rich sources of brominated polyunsaturated lipids. This type of secondary metabolites always exhibited various biological activities ranging from antitumoral, antibacterial, and antifungal, to inhibite pancreatic lipase and HIV-1 integrase [3]. A library of novel brominated polyunsaturated lipids was found and confirmed from the chemical investigation of marine sponge X. testudinaria. Xestonarienes A–H (S18–S25) [21] (Supplementary Fig. S4) and methyl (E, E)-14,14-dibromo-4,6,13-tetradecatrienoate (S26) [22] were isolated from sponge X. testudinaria (collected at Weizhou Island, Guangxi Autonomous Region, China). Another new compound xestonariene I (S27) [23] was obtained from sponge X. testudinaria collected at Ximao Island, in 2014. Brominated polyunsaturated lipids represent a new class of inhibitors of pancreatic lipase (PL), an essential enzyme for efficient fat digestion, since the ethyl xestospongic ester (27) [21] and methyl 22-bromo-(17E,21E)-docosa-17,21-diene-9,11,19-triynoate (28) [23] exhibited significant inhibitory activity against PL with the IC50 values of 3.11 μM and 0.61 μM, respectively. The result was comparable to that of the positive control orlistat (IC50 = 0.78 μM). For structure-activity relationships (SAR) analysis, a terminal (E)-enyne functionality, a diyne within the chain, and methyl ester group are the key functional groups for sustaining the activity of this kind of structure. In addition, another known compounds methyl 18-bromo-(17Z)-octadeca-l7-ene-5,7,15-triynoate (29) [22] and a new steroidal ketone (30) [24] (Fig. 3) from the animal exhibited significant inhibitory activity against PTP1B with the IC50 values of 5.30 μM and 4.27 μM, respectively. Ursolic acid was served as a positive control, and its IC50 value was 2.39 μM.
Structures of new bioactive isolates from sponges.
Six new 3-alkylpyridine alkaloids, topsendines A–F (S28–S33) [25], were isolated from Hainan sponge Topsentia sp. Two new 5-alkylpyrrole-2-carboxaldehyde derivatives, mycalenitrile-15 (31) and mycalenitrile-16 (S34) [26], along with five known related ones, were isolated from the marine sponge Mycale lissochela (Fig. 3 and Supplementary Fig. S5). In bioassay, the new compound 31 and the known compound (6’Z)-5-(23’-cyano-6’-tricosenyl)pyrrole-2-carboxaldehyde (32) [26] (Fig. 3) exhibited significant PTP1B inhibitory activities with the IC50 values of 8.6 and 3.1 μM, respectively, which are comparable with the positive control ursolic acid (IC50 = 3.6 μM). A preliminary SAR analysis revealed that the unsaturated aliphatic side chain was potentially necessary for PTP1B inhibitory activity.
Nitrogenous sesquiterpenoids with cyanide, isocyanide, isothiocyanate, or formamide functionalities, are the secondary metabolites seldom discovered from nature. According to the reports, they were mainly found to exist in the sponges of the order Axinellida. As expected, two new highly oxidized formamidobisabolene sesquiterpenes (S35 and S36) [27], together with four new uncommon nitrogenous eudesmane-type sesquiterpenes, axiriabilines A–D (S37–S40) [28], were isolated from a Hainan sponge Axinyssa variabilis. The absolute configurations of compounds S37 and S40 were determined by TDDFT-ECD calculation.
Spongian diterpenes are a family of isoprenoid natural products displaying parent 6,6,6,5-tetracyclic ring system. Aside from their role as eco-physiological mediators, a broad range of pharmaceutically relevant biological activities such as cytotoxic, antifungal, antiviral, and other biological activity, have been reported for spongian diterpenes, making them attractive targets for chemists. Our group has isolated a series of spongian diterpenes from sponge Spongia officinalis including new compounds, 3-nor-spongiolide A (S41), spongiolides A and B (S42 and S43) [29], as well as two rare new furan butanolides sponalisolides A and B (33 and 34) (Fig. 3 and Supplementary Fig. S6) [30]. Compounds 33 and 34 were further separated to their corresponding enantiomers 33a/33b and 34a/34b, respectively. The absolute configurations of S41–S43 were determined by ECD calculations, whereas the absolute configuration of two pairs of enantiomeric compounds (33a/33b and 34a/34b) was unambiguously established by biomimetic total synthesis. The synthetic route involved a key Johnson-Claisen rearrangement and a lactone cyclization after epoxidation or dihydroxylation (Scheme 2). The natural products (33a/33b and 34a/34b) (Fig. 3) exhibited the anti-quorum sensing activity to the bacteria Pseudomonas aeruginosa.
Biomimetic synthetic route of 33 and 34.
Sponges were the first invertebrates shown to contain sterols. They have been shown to have the most diverse array of novel sterols. In our study, two new C29 steroids with an unusual α-keto-enol functionality bearing A-ring, xidaosterols A (S44) and B (S45) [31], and two new bis-quinolizidine alkaloids, neopetrosiasins A (S46) and B (S47) [32], possessing cis- and trans-quinolizidine nuclei, were isolated from the sponge Neopetrosia chaliniformis (Supplementary Fig. S7). The structures of S46 and S47 were unambiguously determined by extensive spectroscopic data and single-crystal X-ray analyses. Besides, chemical study of a Hainan sponge Halichondria sp. resulted in the isolation of three new sterols, halichsterols A–C (S48–S50) (Supplementary Fig. S7) [33]. Compounds S44 and S45 belong to a small group of steroids that are always found as intermediates in synthesis but also exist in some marine benthic invertebrates. Meanwhile, neopetrosiasins A (S46) and B (S47) are macrocyclic diamine alkaloids, which are a class of structurally interesting marine natural products mainly occurring in sponges. They are regarded to be biogenetically derived from bis-3-alkylpyridine or reduced bis-3-alkylpridine units.
Formamidobisabolene-based sesquiterpenes are a small group of structurally unusual natural products only found from marine sponges and nudibranchs. A chemical study of the marine sponge Halichondria sp. resulted in the isolation of eight new formamidobisabolene-based sesquiterpenes (35, 36, and S51–S56) (Fig. 3 and Supplementary Fig. S8) [34]. In bioassay, halichine C (35) and halichine D (36) (Fig. 3) displayed significant inhibitory effect on LPS-induced NO production in BV-2 microglial cells at 10 μM.
Metabolites of mixed sesquiterpene and quinone or hydroquinone biosynthesis are common in marine sponges. For instance, xishaeleganins A–D (S57, 37, S58, and S59) [35] were isolated from the Xisha marine sponge Dactylospongia elegans (Fig. 3 and Supplementary Fig. S8). Their structural variation mainly focuses on the degree of oxygenation and substitution to the aromatic ring. In addition, xishaeleganins B (37) (Fig. 3) showed significant antibacterial activity against Staphylococcus aureus, with minimum inhibitory concentration (MIC) value of 1.5 μg/mL, which is comparable with that of positive control vancomycin (MIC: 1.0 μg/mL).
Soft corals (Alcyonacea)
Corals are the common group of sessile invertebrates in the ocean. Secondary metabolites from corals have great diversity because these sessile organisms need exceptional chemical weapons for potential parasite predation and microbial colonization. Our group has a great interest in soft corals and has been persistently studying on them for over 20 years. In this section, we will illustrate our mainly achievements on soft corals in the past 10 years.
During the investigation of the soft corals Lobophytum sp. collected at Ximao Island, Hainan Province, China, in October 2013, two unusual steroids, (22R,23S)-3β-hydroxy-23-methyl-17,20-epoxyergost-5-en-22-yl acetate (S60) and (22R,23S)-5-hydroperoxy-23-methyl-5α-17,20-epoxyergost-6-ene-3β,22-diol (38), were obtained (Fig. 4 and Supplementary Fig. S9) [36]. The chemical structure including the absolute configuration of compound S60 was further confirmed via chemical correlation with the related known one (S61). In bioassay, compound 38 showed considerable NF-кB inhibitory activity with the IC50 value of 8.96 μg/mL. Considering the surprising structural properties and biological activity of these compounds, we resampled Lobophytum sp. from Weizhou Island, in May 2015. The chemical study of the second collection led to the isolation of four new polyhydroxylated steroids (S62–S65) (Supplementary Fig. S9) [37], together with three new capnosane-type diterpenoids (39, S66, and S67) (Fig. 4 and Supplementary Fig. S10) [38]. It is worth mentioning that capnosane-type diterpenoid is a group of uncommon derivatives. This is the first report of capnosanes from the Lobophytum sp. [38]. In addition, nine new bicyclic cembranoid ethers, lobophytolins A–I (40–44 and S68–S71), and one new prenylated-guiane-type diterpene lobophytolin J (45) have been isolated from the soft coral Lobophytum sp. (collected off Xisha Island, Hainan province, China) (Fig. 4 and Supplementary Fig. S11) [39, 40]. Quantum mechanical (QM)-NMR method was successfully used to complete the stereochemical assignment of 40–45 and S68–S71 with the DP4 + and the iJ/dJ-DP4 approaches. In the cases of 40 and 41, the application of J-DP4 displayed better performance than DP4 + method in the assignment of relative configurations of multi-stereogenic centers, which was supported by X-ray crystallography [40]. The absolute configuration of lobophytolin H (44) was determined by the application of the modified Mosher’s method and chemical transformation. In bioassay, lobophytolin D (43) (Fig. 4) exhibited promising cytotoxicity against HT-29, Capan-1, A549, and SNU-398 human cancer cell lines with the IC50 values of 4.52, 6.62, 5.17, and 6.15 μM, respectively [39].
Structures of representative compounds from soft corals of Lobophytum.
In the chemical study of the soft coral L. crassum (collected off Ximao Island, in May 2014), a series of polyoxygenated cembranoids, lobophycrasins A–D (46, 47, S72, and S73), (-)-humilisin A (S74), lobocrassins G and H (S75 and 48), 6-oxo-cembrene-A (S76), and 14-epi-lobophytolide B (S77), were isolated and identified (Fig. 4 and Supplementary Fig. S12) [41, 42]. Among them, compound 46 is a C-16 norcembranoid and 48 is a C-4 norcembranoid. In addition, the structure of lobocrasol (49) was firmly revised based on X-ray diffraction analysis. By comparing the major chemical components in the soft corals of Lobophytum collected four times, their metabolites type varied widely, which may be caused by the geographical and seasonal factors of the collection, as well as interspecies differences.
The soft corals of Sinularia are well known as a produce factory of terpenoids, and in our ongoing research on this genus for the past decade, they were the most productive source for searching of novel compounds. For example, five different types of novel terpenoids, sinulatumolins A–E (50, S78, and 51–53), were isolated from the South China Sea soft coral S. tumulosa [43]. Sinulatumolin A (50) represented the first example of sesquiterpene bearing an eight-membered cyclic peroxide ring from soft coral, and 51 represented the second furanosesquiterpenoid with a 2-methylfuran-3(2H)-one moiety (Fig. 5). In the anti-inflammatory activity evaluation, compounds 50 and 51–53 displayed significant TNF-α inhibitory activity with the IC50 values of 7.5, 2.6, 5.5, and 3.6 μM, respectively, being comparable with that of the positive control dexamethasone (IC50 = 8.7 μM). Six novel asteriscanoids, sinuhumesins A–F (54, and S79–S83) and two rare polycyclic merosesquiterpenoids, (+)-9-epi-verrubenzospirolactone (55) and (–)-9-epi-verrubenzospirolactone (56), were isolated from Hainan soft coral S. humesi [44]. Compounds 55 and 56 were a pair of enantiomers further separated by chiral HPLC. Sinuhirtins A (57) and B (S84) were two new uncommon norhumulene-type norsesquiterpenoids isolated from the soft coral S. hirta (Fig. 5 and Supplementary Fig. S13) [45].
Structures of representative sesquiterpenoids from soft corals of Sinularia.
Cembrane-type diterpenoids are one class of the conspicuous secondary metabolites widely distributed in the soft corals. The intriguing patterns of different substitutions diversify types of cembranoids. Six novel α-methylene-δ-lactone-bearing cembranoids (58 and S85–S89), together with one 15-membered macrocyclic diterpenoid (59), and one rare biscembranoid (60) were isolated from the soft coral S. flexibilis [46]. The structure of 60 was unambiguously confirmed by X-ray diffraction analyses. Epoxyfexibilene (59) represents the second flexitilane-type diterpenoid discovered from marine sources. Sinulafexiolide L (60) is the third member of the rare cembrane dimer connected through a C–C single bond (Fig. 6). The chemical investigation of soft coral S. flexibilis collected off the coastline of Hainan Island led to the isolation of three new cembranoid esters, xidaosinularides A–C (61, S90, and S91), featuring an n-butyl alcohol moiety [47]. It is worth noting that not only the butyl ester group at C-16 was uncommon, but also the configuration at C-1 position was an unusual β-oriented. According to the Tursch’s empirical rule, isopropyl moieties of cembranoids from Alcyonacean soft corals are always α-oriented, while those from Gorgonacean corals are always β-oriented. Besides, a novel norditerpenoid, sinusiaetone A (62), featuring an unprecedented bicyclo[11.3.0]hexadecane carbon skeleton, and two new polyoxygenated cembranoids, sinusiaeolide A (S92) and sinusiaesin A (S93), were isolated from the Hainan soft coral S. siaesensis (Fig. 6 and Supplementary Fig. S14) [48]. These compounds (62, S92, and S93) displayed a significant inhibitory activity against lipopolysaccharide-induced inflammation in BV-2 microglial cells.
Structures of representative Cembrane diterpenoids and related rare diterpenoids (62, 71 and 72) from soft corals of Sinularia.
The study of soft corals Sinularia sp., which were collected from the Xisha Island, led to the isolation of four new cembranoids (63, S94, 64, and S95) [49]. The absolute configuration of 63 was established by X-ray diffraction analysis. Compounds 63 and 64 (Fig. 6) displayed moderate inhibitory activity against Aβ42 aggregation without cytotoxicity, suggesting that these cembranoids as new anti-Aβ aggregation agents, provided a novel chemical scaffold for anti-Alzheimer’s disease drug discovery.
Four other new cembranoids, sinulacrassins A−C (S96, 65 and S97) and ent-xishaflavalin G (S98), have been discovered from S. crassa [50]. The present results highlighted the unusual coexistence of α (S97 and S98) and β (S96 and 65) configurations of C-1 in cembranoids from soft coral in the Order Alcyonacea. As mentioned above, Tursch’s empirical rule is generally accepted and applied for deducing the absolute configuration of C-1 in cembranoids. However, in view of the reports regarding the co-existence of 1-α and 1-β series of cembranoids from Order Alcyonacea, we have to use this empirical rule more carefully. The bioassay results revealed that compound 65 (Fig. 6) was a novel α-glucosidase inhibitor with the IC50 value of 10.65 μM [50]. In the study of soft corals S. scabra (collected off Xigu Island, Hainan Province) [51, 52], six new cembranoids (66–69, S99, and S100) and one new polycyclic furanobutenolide-derived norcembranoid (S101) [52] were isolated and determined (Fig. 6 and Supplementary Fig. S15). Xiguscabrate B (66), xiguscabrols A and B (67 and 68), and 8-epi-xiguscabrol B (69) (Fig. 6) exhibited strong inhibitory activity on the proliferation of ConA-induced T lymphocyte cells with the IC50 values ranging from 2.3–8.4 μM [51]. The result gave an inspiration for the discovery of novel immunosuppressive agents.
In addition, a series of novel cembranoids (S102–S111) with hydroxyl or epoxy substitutions were discovered by the chemical study on the soft coral S. nanolobata [53, 54]. The absolute stereochemistry of ximaonanolobatin A (S102) was determined by X-ray diffraction analysis. The absolute configuration of ximaonanolobatin B (S103) was established by QM-NMR calculations and chemical transformation, whereas the absolute configuration of ximaonanolobatin C (S104) was determined using the modified Mosher’s method. A detailed chemical investigation of soft coral S. humilis led to the isolation of other four new cembranoids (70 and S112–S114), together with two new uncommon diterpenoids humilisins E and F (71 and 72) (Fig. 6 and Supplementary Fig. S16) [55]. Humilisin A (70) was a distinct cembranoid with an ether linkage between C-3 and C-7, and was firstly reported by our group. In bioassay, Compound 72 (Fig. 6) displayed a significant inhibitory effect on LPS-induced inflammatory response (NO production) in BV-2 microglial cells.
Casbane diterpenes are featured by the presence of a dimethyl-cyclopropyl moiety fused to the 14-membered ring, which are extremely rare in nature and marine organisms. From South China Sea soft corals, a series of novel casbane-type diterpenoids were obtained, which greatly expanded the diversity and complexity of casbane family. For example, three rare casbane diterpenoids with an uncommon 8,10-peroxide bridge, sinuereperoxides A–C (73–75), together with other six new casbanes (76–79, S115, and S116) were isolated from the soft coral S. erecta [56, 57]. Their structures and absolute configurations of 73–75 (Fig. 7) were determined by X-ray diffraction analysis, whereas the absolute configurations of 76–79, S115, and S116 were determined by TDDFT-ECD calculations. In bioassay, compounds 73, 75 and 79 (Fig. 7) exhibited considerable anti-inflammatory activity by inhibition of TNF-α release, with the IC50 values of 10.6 μM, 33.8 μM and 5 μM, respectively. The chemical study on the soft coral S. crassa also led to the isolation and characterization of eleven new casbane-type diterpenoids, sinucrassins A–K (80, 81, and S117–S125) [58]. Among them, the absolute configurations of 80 and 81 were determined by X-ray diffraction analysis, whereas the absolute configurations of S122–S125 were determined by TDDFT-ECD calculations. The general rule that diagnostic 13C NMR chemical shifts of the geminal methyls are very close in the trans-isomer, while very distinct in the cis-isomer, are helpful to determine the relative configurations of C-1/C-2 in casbanes. Other two new casbanes (82 and 83) [59] with the oxidation at C-16 were isolated from soft coral S. nanolobata (Fig. 7). Through a series of chemical reactions, compound 83 was eventually associated with 82 (Scheme 3). Therefore, its stereochemistry was further confirmed same as that of 82, which had been unambiguously determined by a successful performance of X-ray crystallography. In the anti-inflammatory assay, compounds 82a, 83, and 83a displayed inhibitory activity on NO production against LPS-induced inflammation-related BV-2 microglial cells at the concentration of 20 μM, which were comparable to that of the positive control resveratrol [59].
Structures of representative Casbane diterpenoids and related rare diterpenoids (84 and 85) from soft corals of Sinularia.
Chemical correlation of compounds 82 and 83.
Interestingly, sinueretone A (84), featuring an unprecedented tricyclo[12.1.0.05,9]pentadecane carbon framework, and sinunanolobatone A (85), featuring an unprecedented bicyclo[13.1.0]pentadecane carbon framework, were also isolated from the soft coral S. erecta and S. nanolobata, respectively (Fig. 7) [56, 59]. Combined with the biosynthesis of cembrane-type and casbane-type diterpenes from geranylgeranyl pyrophosphate [60], the biosynthetic connection of these diterpenoids was described as shown in Scheme 4. In addition, compound 85 displayed inhibitory activity on NO production against LPS-induced inflammation-related BV-2 microglial cells at the concentration of 20 μM. It significantly reduced the mRNA transcription levels of the pro-inflammatory cytokines IL-6 and IL-1β in LPS stimulated BV-2 microglial cells, which further demonstrated the anti-inflammatory effect of compound 85 [59].
The plausible biosynthetic connection of cembranes, casbanes, sinueretone A (84) and sinunanolobatone A (85).
Moreover, some low abundance diterpenoids were discovered occasionally. For example, three complex polyoxygenated possessing uncommon tetradecahydro2,13:6,9-diepoxybenzo[10]annulene scaffold, namely ximaoornatins A–C (86–88), and one new eunicellin-type diterpene, litophynin K (89) (Fig. 8), were isolated from the soft coral S. ornate [61]. Sinuhumilol A (90) was a new capnosane-type diterpenoid isolated from the soft coral S. humilis [62]. The chemical investigation of the Xisha soft coral S. polydactyla has led to the isolation of another new capnosane-type diterpenoid sinulacetate (91), as well as a new prenyleudesmane-type diterpene sinupol (92), three new lobane-type diterpenes 13-methoxyloba-8,10,15(16),17(18)-tetraene (93), 8,10,13(15)Z,16E-lobatetraene (94), and 19-hydroxy-lobatetraene (95) (Fig. 8). It is noteworthy that three new diterpenes with new structural skeleton, xishacorenes A–C (96–98) (Fig. 8), featuring an undescribed bicyclo[3.3.1]nonane nucleus bearing 1-vinyl and 13-[(E)-4-methylpenta1,3-dien-1-yl] alkyl chains, were also discovered from the S. polydactyla [63,64,65]. The bioassay results showed sinulacetate (91) and sinupol (92) exhibited promising PTP1B inhibitory activities [63]. Xishacorenes A–C (96–98) exhibited a dose-dependent promotion effect on the ConA-induced T lymphocyte proliferation [65]. In addition, the fascinating molecular architectures and potential pharmaceutical applications of 96–98 have attracted considerable interest of synthetic chemists for total chemical syntheses. Sarpong group have successively completed the total synthesis of (-)-xishacorene B from (R)‑carvone, as well as bio-inspired synthesis of xishacorenes A–C from fuscol [66,67,68,69]. Moreover, they have described immunomodulatory activity studies of fuscol and xishacorenes. These observations suggest that hydrophilicity of the xishacorenes should be enhanced to improve the immunomodulatory potency [67].
Structures of other uncommon diterpenoids (86–98) from soft corals of Sinularia.
(2β,3β,4α,5α,8β)-4-methylergost-24(28)-ene-2,3,8-triol (S126) and (3β,7α)-24-methyl-7-hydroperoxycholest-5,24(28)-diene-3-ol (S127) were two new steroids isolated from the soft coral S. depressa Tixier-Durivault (collected off Lingshui Bay, Hainan Province) [70]. Three new oxygenated steroids, sinulasterols A–C (S128–S130), were also isolated from the soft coral S. depressa (collected off Ximao Island) [71]. Among them, Sinulasterols A and B (S128 and S129) are featured with unusual C-18 oxygenated patterns. Two new polyhydroxylated steroids, 7α-hydroxy-crassarosterol A (S131) and 11-acetoxy-7α-hydroxycrassarosterol A (S132), were derived from the soft corals S. flexibilis [72] (Supplementary Fig. S18). The stereochemistry of S132 was established same as that of S131 through chemical conversion. In the study of soft coral Sinularia sp. collected from the Xisha Islands, two new highly oxygenated ergostane-type sterols (99 and 100) (Fig. 9) were isolated and identified [73]. In bioassays, 99 and 100 showed antiproliferative activity against a panel of cancer cell lines, including MDA-MB-436, A549, Hep3B, HT-29, and H157 cell lines. Besides, Western blot assay showed that 99 increases the expression of Bax and down-regulates the expression of Bcl-2 [73], which suggests compound 99 exhibited the anticancer potential by initiating apoptosis process. A new 5α,8α-epidioxysterol, yalongsterol A (S133), was isolated from the soft coral Sinularia sp. that was collected off Yalong Bay, Hainan Province [74]. Two new steroids featuring a different C-20 side chain, ximaosteroids E (101) and F (102) (Fig. 9), were discovered from the soft coral Sinularia sp. (collected off the coast of the Ximao Island), with significant cytotoxicity against the HL-60 tumor cells with the IC50 values of 1.79 and 4.03 μM, respectively [75]. In addition, a pair of epimers of novel highly degraded steroid derivatives, namely erectsterates A and B (103 and 104) (Fig. 9), have been also obtained under the chemical investigation of soft coral S. erecta [76]. Their structures were established by extensive spectroscopic analysis and deduction from biosynthesis route. The B ring of steroidal nucleus was completely broken by twice cleavages of C-C bonds, and then the C ring was oxidized by Baeyer-Villiger reaction to form an unprecedented seven-membered lactone moiety in ring C of steroid, and then, the A ring and C ring were connected by an ester bond.
Structures of novel representative steroids from soft corals of Sinularia.
Sarcophyton is a genus of soft corals in the family Alcyoniidae. As a hardy and dominant soft coral genus in many coral reef areas of China, they are the main source of biscembranoids (Fig. 10) generated by Diels-Alder cycloaddition. During our ongoing search for these compounds, many species in this genus were systematically investigated. Four new biscembranoids, bislatumlides C–F (105, S134–S136), were isolated from the Hainan soft coral S. latum [77]. The absolute configurations of bislatumlides C and E (105 and 106) were determined by TDDFT-ECD calculation, which resulted in the confirmation of the absolute configurations of S134-S137 by comparison of the CD spectra. The Scheme 5 illustrated the formation of these biscembranoids. Briefly, the Δ1(2) double bond in the α,β-unsaturated γ-lactone ring as a dienophile group was reacted with a trisubstituted conjugated Δ21(34)/Δ35(36)-butadiene moiety. An endo-cycloaddition generated 105, S134, S136, and S137, whereas an exo-cycloaddition produced 106 and S135.
Structures of novel representative biocembranoids from soft corals of Sarcophyton.
The plausible endo/exo-Diels-Alder Cycloaddition.
Because of the complexity of the dimeric cembranoids, some confusions were inevitable. For instance, the structure of methyl tortuoate D was firstly isolated and reported as 107a. However, in our study of the Hainan soft coral S. tortuosum, the planar structure of tortuoate D was identified as 107 [78]. In addition, lobophytone K (107b) isolated from Hainan soft coral L. pauciflorum by Lin et al., was proved to be the same compound as 107 and 107a by our group through an extensive analysis and comparison of their NMR data and the optical rotation values. Later, other five novel biscembranoids (S138–S142) were also isolated from the soft coral S. tortuosum (Supplementary Fig. S19) [79]. In bioassay, ximaolides I (S139), and K (S141) exhibited significant inhibition activity against LPS-induced TNF-α release in RAW264.7 macrophages.
The study of S. trocheliophorum Marenzeller also led to the discovery of an unprecedented biscembranoid bissartrolide (108) (Fig. 10). Unlike the dimers mentioned above, it was formed by an esterification rather than a Diels-Alder reaction. The sartrolides A–G (109, 110, and S143–S147) (Supplementary Fig. S20) were a series of novel cembranolides containing α,β-unsaturated ε-lactone that were also obtained from the S. trocheliophorum [80]. The sartrolides differed from each other at the partial structure from C-1 to C-8 with various substitutions. Sarcophytonolides N–R (111 and S148–S151) (Supplementary Fig. S20) were another group of novel cembranolides isolated from the soft coral S. trocheliophorum Marenzeller, their structures have been elucidated by detailed spectroscopic analysis [81]. Sarcophytonolide N (109) (Fig. 11) showed significant inhibitory activity toward PTP1B enzyme with the IC50 value of 5.95 μM. In addition, the chemical investigation of this soft coral also yielded two new unprecedented diterpenoids (112 and 113) possessing a tetradecahydrocyclopenta[3′,4′]cyclobuta[1′,2′:4,5]-cyclonona[1,2-b]oxirene ring system, along with their probable biogenetic precursor, sarcophytonolide M (114). Two new sarsolenane diterpenes, dihydrosarsolenone (115), methyl dihydrosarsolenoneate (116), and two new capnosane diterpenes, sarsolilides B (117) and C (118) were discovered from the same species 1 year later [82, 83]. It is worth noting that compound 113 and 117 exhibited significant inhibitory activity against PTP1B, which were comparable to the positive control oleanolic acid [82]. In order to examine whether seasonal factors can lead to differences in metabolites of the same species, the soft corals S. trocheliophorum Marenzeller were recollected in different season, resulting in two hydrocarbon cembranoids, yalongenes A (119) and B (S152) [84]. Yalongene A (119) (Fig. 11) showed a significant cytoprotective activity on H2O2 induced SH-SY5Y cell injury model at the concentration of 1 µM. In the further investigations of soft corals S. trocheliophorum, a new 9,11-secosteroid (120) [72], three new capnosane-type diterpenoids (S153–S155) [85], together with a set of new cembranoids (S156–S181) [86,87,88,89,90] were isolated and characterized. Interestingly, sarcophytrols M–U (S165–S173) exhibit a variety of cyclization patterns, including furan, pyran, oxepane, or peroxyl rings, which provide in-depth understanding of the diversity of cyclized cembranoids [87]. Sartrolides H–J (S177–S179) were distinguished by an unusual α,β-unsaturated ε-lactone (Supplementary Fig. S20) [89]. The discovery of these highly oxidative cembranoids enriched the family of cembranoids derived from the soft coral S. trocheliophorum.
Structures of some representative compounds from soft corals of Sarcophyton.
The chemical study on other species of the genus Sarcophyton was also very productive. Sixteen new cembranoids (S182–S197) were isolated from the soft coral S. ehrenbergi [91, 92]. Their structures including absolute configurations were established by a combination of detailed spectroscopic analysis, comparison with reported data, modified Mosher’s method, TDDFT-ECD calculations and/or X-ray diffraction analysis. Sarcoehrenolides A–E (S182–S186) are featured by an α,β-unsaturated γ-lactone moiety at C-6 to C-19 (Supplementary Fig. S21) [91]. In the TNF-α inhibitory biotest, compound S183 exhibited a potent inhibitory activity with the IC50 value of 8.5 μM, which was analogous to the positive control dexamethasone (IC50 = 8.7 μM) [91]. Ximaoglaucumins A − F (S198–S203) [93], and ximaocembrols A, B and (±)-ximaocembrol C (S204–S207) [94], were isolated from the soft corals S. glaucum and S. crassocaule, respectively. Although the determination of the stereochemistry of cembranoids is always a challenging task without suitable single crystals, a series of reliable approaches including extensive spectroscopic analysis, quantum chemical calculations, modified Mosher’s method, and Snatzke’s method were applied in combination. Finally, their stereochemistry was unambiguously confirmed as shown in Supplementary Fig. S22. In the case of S. mililatensis, a novel diterpenoid, sarcomililate A (121), possessing an unprecedented tricyclo[11.3.0.02,16]-hexadecane scaffold, as well as its possible biogenic precursors, sarcomililatols A and B (122 and 123) (Fig. 12), was isolated from the samples collected from Hainan Province [95]. The chemical structure including absolute configuration of 121 was unambiguously determined by a combination of residual dipolar coupling (RDC)-based NMR analysis, TDDFT-ECD calculation, and Snatzke’s method. The absolute configuration of 121 was further confirmed by a comparison with 122, whose absolute configuration was determined by X-ray diffraction. The plausible biogenetic relationship of 121 − 123 was depicted in Scheme 6, which further corroborated the confirmation of absolute configuration of 121 and 123. The study of S. infundibuliforme also led to the discovery of two new nitrogenous diterpenoids, sarinfacetamides A (124) and B (125), featuring an uncommon tricyclo[6.3.1.01,5]dodecane scaffold (Fig. 12). As shown in Scheme 7, a plausible biosynthetic pathway for 124 and 125 from co-isolated known compound nanolobatin B was also proposed. Moreover, sarinfacetamide A (124) exhibited an interesting promotion effect on the ConA-induced T lymphocyte proliferation with a proliferation rate of 36.18% at the concentration of 10 μM [96].
Structures of compounds 121–125.
Proposed biosynthetic pathway of compound 121.
Proposed biosynthetic pathway of compounds 124 and 125.
As mentioned above, the soft corals of Genera Lobophytum, Sinularia, and Sarcophyton are dominant cnidaria inhabiting South China Sea and consequently being extensive resources in the subject of marine natural product chemistry. Apart them, there are also some relatively less populated soft corals, such as Litophyton nigrum, Lemnalia flava, Clavularia viridis, Cladiella krempfi, and Klyxum flaccidum being collected and chemical investigation. The chemical investigation of the Xisha soft coral L. nigrum has resulted in the isolation of eight new nardosinane-type sesquiterpenoids (126, 127, and S208–S213), four new neolemnane-type sesquiterpenoids (128, 129, S214, and S215), as well as one uncommon sesquiterpenoid dimer (130) (Fig. 13 and Supplementary Fig. S23) [97,98,99]. Notably, linardosinene A (126) and lineolemnene D (129) represent uncommon nornardosinane and seconeolemnane sesquiterpenoids, respectively [97]. In addition, the bioassay results indicated that the compound (127) exhibited potent PTP1B inhibitory activity (IC50 = 0.67 μg/mL) compared to the positive control [99].
Structures of representative compounds from soft corals Litophyton nigrum, Lemnalia flava, Clavularia viridis, Cladiella krempfi, and Klyxum flaccidum.
A detailed chemical investigation of the Xisha soft coral L. flava led to the acquisition of four new nardosinane-type sesquiterpenoids (S216 − S219), a new neolemnane-type sesquiterpenoid (S220), a new sesquiterpenoid (S221), and two new cembranoids (S222 and S223) (Supplementary Fig. S24) [100, 101]. Unlike xishaflavalin E (S220), the xishaflavalin F (S221) featured an uncommon 6/9 fused bicyclic skeleton. One point to note is that the discovery of cembrane-type diterpenes from the genus Lemnalia was reported for the first time [100].
Another Xisha soft coral C. viridis has been well studied, and finally yielded two new trinor-guaiane sesquiterpenes (S224 and S225) [102], four new halogenated laurane-type sesquiterpenoids (131 − 133 and S226) [103], one new aromadendrane-type sesquiterpenoid (S227) [103], and thirteen dolabellane-type diterpenoids (134 and S228–S239) [104] (Fig. 13 and Supplementary Fig. S25). Among them, ent-laurenisol (133), and clalaurenol B (S226) had also been produced by the soft coral L. flava [103]. The structure including absolute configuration of clavuridin B (S224), clavurol F (S235) and clavirolide I (S239) was directly determined by X-ray diffraction analysis [102, 105]. Most notably, clavuperoxylides A and B (S231 and S232) and clavufuranolides A − C (S236–S238) exhibited the structural diversity of the dolabellanes comprising peroxyl group, novel peroxide bridge, and tetrahydrofuran ring [105]. In bioassay, sesquiterpenoids isobromolaurenisol (131), clalaurenol A (132), ent-laurenisol (133) and clavurol E (134) exhibited significant inhibitory activities against PTP1B [105]. Meanwhile, 131 − 133 (Fig. 13) showed potential anti-inflammatory activity in vitro by inhibiting the NF-κB signaling pathway [103].
Our investigation on the chemical constituents of the soft coral C. krempfi, collected off the Weizhou Island, yielded seven new eunicellin-based diterpenoids (S240–S243, and 135–137) [106, 107]. It is well known that eunicellins represent the largest class of 2,11-cyclized cembranoids and share a common 15-oxatricyclo[6.6.1.02,7]pentadecane system [5]. By a network of chemical conversions of S240–S243 and 135, together with detailed spectroscopic analysis and comparison, the stereostructures of these isolates were all elucidated (Supplementary Fig. S26). In bioassay, 135–137 (Fig. 13) displayed moderate anti-inflammatory effect [106]. In addition, twenty polyoxygenated eunicellin diterpenoids (138 and S244–S262), and two novel polyoxygenated diterpenoids, klyflaccilides A (139) and B (140) (Fig. 13 and Supplementary Fig. S26), featuring an uncommon 6/5/8/3 tetracyclic ring system, were isolated from the Hainan soft coral K. flaccidum [108, 109]. It was reasonable to speculate that 139 and 140 were derived from klyflaccilin A (138) based on the common fragment [109].
Mollusks
Marine mollusks, belonging to the second largest invertebrate phylum (Mollusca), comprise a group of shelled and shell-less soft bodied animals that are not only highly diverse in size and anatomical structure, but also in their behavior and habitat. Marine mollusks usually produce structurally diverse polyketides, polypropionates terpenes, and nitrogenous metabolites as chemical defense, which may be attributed to the predator-prey relationship between mollusks and algae, sponges, and corals. Nudibranchs are a family of Opisthobranchia, which are most extensively studied from the natural product chemistry point of view. Many of them are slow-moving, brightly colored, and shell-less slug, and appear to be free of predation causing great interest to biologists, chemists, pharmacologists.
In the several studies [110,111,112] of the South China Sea nudibranch Jorunna funebris and its possible sponge-prey Xestospongia sp., a series of isoquinolinequinone alkaloids, including four renieramycin-type bistetrahydroisoquinolinequinone alkaloids, fennebricins A–D (S263 and 141–143), and N-formyl-1,2-dihydrorenierol (144), were isolated and elucidated as new compounds (Fig. 14 and Supplementary Fig. S27). S263 and 141 are structurally related to the ecteinascidins and the saframycins that are two groups of promising antimicrobial and antitumor alkaloids. However, since these two compounds were only available in trace amount and were relatively unstable, their bioactivity have been unable to determine. But in the case of 142 and 143, they showed strong NF-κB inhibitory activity, indicating a promising anti-inflammatory potential. Very interestingly, we have isolated multiple metabolites occurred simultaneously in both mollusk J. funebris and its associated prey, the sponge Xestospongia sp., suggesting the prey-predator relationship between the two animals.
Structures of representative compounds from nudibranches.
The study on two South China Sea nudibranchs Phyllidiella pustulosa and Phyllidia coelestis, as well as their possible sponge-prey Acanthella cavernosa led to the isolation of nitrogenous cadinane-type sesquiterpenoid xidaoisocyanate A (145), one new naturally occurring nitrogen-containing kalihinane-type diterpenoid bisformamidokalihinol A (146), along with other known nitrogenous terpenoids [113]. By comparison of the typical isolates from the three animals, as well as the previous investigation of the marine sponge A. variabilis from the same sea area, the interesting predator-prey relationship between two nudibranchs and two sponges were considered reasonably. We have also investigated nudibranch Hexabranchus sanguineus and its possible sponge-prey A. cavernosa. Fifteen new nitrogenous sesquiterpenoids, namely ximaocavernosins A–O (S264–S276, 147, and 148) (Fig. 14 and Supplementary Fig. S28), together with other known related compounds were isolated [114]. And a detailed investigation of the Weizhou nudibranch Glossodoris atromarginata yielded a new spongian‐type diterpene (149) (Fig. 14) [115]. In short, the results of above studies suggest that nudibranchs perhaps accumulate the useful dietary metabolites from the sponges, especially those toxic isocyanide derivatives, to be employed as their own chemical defensive agents for surviving in the harsh marine environment.
It is noteworthy that the research of another mollusk of Opisthobranchia has yielded significant findings. From a chemical perspective, the marine sacoglossan Placobranchus ocellatus were collected from the shallow water of Ximao Island, producing a series of racemic non-γ-pyrone polyketides with novel skeletons, ocellatusones A–D (150–153) (Fig. 15) [116], characterized by abicyclo[3.2.1]octane (150, 151), a bicyclo[3.3.1]nonane (152) and a mesitylene-substituted dimethylfuran-3(2H)-one core (153). Some algae-feeding marine sacoglossan mollusks possess the capabilities to photosynthesize through the phenomenon of kleptoplasty. For example, the biosynthesis of the common metabolites, such as γ-pyrone-containing polypropionates, involved photoinduced cyclization. After a literature research on γ-pyrone-containing polypropionates, we have proposed a photobiosynthetic pathway towards these novel polyketides 150–153 (Scheme 8). As expected, the proposed rearrangement through an unprecedented acid induced cascade reaction was further confirmed by successful biomimetic semisynthesis of ocellatusone A (150) from natural precursor 154 (Scheme 9). In addition, the by-product 155 generated from the reaction is also present in the crude extract of the mollusk.
Structures of compounds 150–153 isolated from the marine sacoglossan Placobranchus ocellatus.
Proposed photobiosynthetic pathway towards novel polyketides 150–153.
Biomimetic semisynthesis of ocellatusone A (150) from natural precursor 154.
As mentioned above, the marine pulmonate Onchidium sp. should be of capacity to photosynthesize as it feeds mainly on benthic algae. The discovery of bis-γ-pyrone polypropionates from the animal is strong supporting evidence for the suspicion. Briefly, a dozen of bis-γ-pyrone polypropionates including three new members, 16-epi-onchidione (156) [117], 4-epi-onchidione (157) [117], and 4,16-di-epi-onchidiol (158) [118] were identified from Onchidium sp. (Fig. 16). Many of isolates exhibited a wide range of cytotoxicity [117], implying that the animal photosynthesizes these compounds for chemical defense against predators and survival from the harsh environment.
Structures of compounds 156–158 isolated from the marine pulmonate Onchidium sp.
Conclusion
This review summarizes representative substances from Chinese marine plants and invertebrates discovered by our group in the past decade. These structurally and biologically interesting marine metabolites, along with the rapid development of the technologies on the high-throughput biological screening, their total syntheses and SAR analyses, would greatly benefit the discovery of pharmaceutically interesting lead compounds. Recent years, more and more attentions have been focused on the chemistry and biology of the microorganisms derived from marine plants and invertebrates, resulting in the discovery of a large number of bioactive secondary metabolites. Therefore, the application of multidisciplinary field, including genome mining, biosynthesis, and isotope labeling, will be effective ways to understand the origin and the biosynthetic pathway of the bioactive metabolites, and then, illustrate the relationship between the marine plants, invertebrates, and their associated microorganisms. Furthermore, with the advances of molecular biology, it will greatly increase the speed of finding pharmacological targets for these active molecules.
References
Montaser R, Luesch H. Marine natural products: a new wave of drugs? Future Med Chem. 2011;3:1475–89.
Jiang CS, Muller WE, Schroder HC, Guo YW. Disulfide- and multisulfide-containing metabolites from marine organisms. Chem Rev. 2012;112:2179–207.
Zhou ZF, Menna M, Cai YS, Guo YW. Polyacetylenes of marine origin: chemistry and bioactivity. Chem Rev. 2015;115:1543–96.
Cai YS, Guo YW, Krohn K. Structure, bioactivities, biosynthetic relationships and chemical synthesis of the spirodioxynaphthalenes. Nat Prod Rep. 2010;27:1840–70.
Li G, Dickschat JS, Guo YW. Diving into the world of marine 2,11-cyclized cembranoids: a summary of new compounds and their biological activities. Nat Prod Rep. 2020;37:1367–83.
Shen SM, Appendino G, Guo YW. Pitfalls in the structural elucidation of small molecules. A critical analysis of a decade of structural misassignments of marine natural products. Nat Prod Rep. 2022. https://doi.org/10.1039/d2np00023g.
Zhou ZF, Guo YW. Bioactive natural products from Chinese marine flora and fauna. Acta Pharmacol Sin. 2012;33:1159–69.
Liu DQ, Mao SC, Zhang HY, Yu XQ, Feng MT, Wang B, et al. Racemosins A and B, two novel bisindole alkaloids from the green alga Caulerpa racemosa. Fitoterapia. 2013;91:15–20.
He WF, Yao LG, Liu HL, Guo YW. Thunberol, a new sterol from the Chinese brown alga Sargassum thunbergii. J Asian Nat Prod Res. 2014;16:685–9.
Yu XQ, He WF, Liu DQ, Feng MT, Fang Y, Wang B, et al. A seco-laurane sesquiterpene and related laurane derivatives from the red alga Laurencia okamurai Yamada. Phytochemistry. 2014;103:162–70.
Li XL, Kurtan T, Hu JC, Mandi A, Li J, Li XW, et al. Structural and stereochemical studies of laurokamurols A-C, uncommon bis-sesquiterpenoids from the Chinese red alga Laurencia okamurai Yamada. J Agric Food Chem. 2017;65:1550–5.
Li XL, He WF, Li J, Lan LF, Li XW, Guo YW. New laurane-type sesquiterpenoids from the Chinese red alga Laurencia okamurai Yamada. J Asian Nat Prod Res. 2015;17:1146–52.
Zhou ZF, Kong LY, Kurtan T, Liu HL, Mandi A, Li J, et al. Four phragmalin orthoesters from the Chinese mangrove Xylocarpus granatum. Planta Med. 2014;80:949–54.
Zhou ZF, Kurtan T, Mandi A, Gu YC, Yao LG, Xin GR, et al. Novel and neuroprotective tetranortriterpenoids from Chinese mangrove Xylocarpus granatum Koenig. Sci Rep. 2016;6:33908.
Zhou ZF, Taglialatela-Scafati O, Liu HL, Gu YC, Kong LY, Guo YW. Apotirucallane protolimonoids from the Chinese mangrove Xylocarpus granatum Koenig. Fitoterapia. 2014;97:192–7.
Zhou ZF, Liu HL, Zhang W, Kurtán T, Mándi A, Bényei A, et al. Bioactive rearranged limonoids from the Chinese mangrove Xylocarpus granatum Koenig. Tetrahedron. 2014;70:6444–9.
Cai YS, Sun JZ, Tang QQ, Fan F, Guo YW. Acanthiline A, a pyrido[1,2-a]indole alkaloid from Chinese mangrove Acanthus ilicifolius. J Asian Nat Prod Res. 2018;20:1088–92.
Xue DQ, Mao SC, Yu XQ, Guo YW. Isomalabaricane triterpenes with potent protein-tyrosine phosphatase 1B (PTP1B) inhibition from the Hainan sponge Stelletta sp. Biochem Syst Ecol. 2013;49:101–6.
Zhao ZB, Sun JZ, Mao SC, Guo YW. Fasciospyrinadine, a novel sesquiterpene pyridine alkaloid from a Guangxi sponge Fasciospongia sp. J Asian Nat Prod Res. 2013;15:198–202.
He WF, Xue DQ, Yao LG, Li JY, Li J, Guo YW. Hainanerectamines A–C, alkaloids from the Hainan sponge Hyrtios erecta. Mar Drugs. 2014;12:3982–93.
Liang LF, Wang T, Cai YS, He WF, Sun P, Li YF, et al. Brominated polyunsaturated lipids from the Chinese sponge Xestospongia testudinaria as a new class of pancreatic lipase inhibitors. Eur J Med Chem. 2014;79:290–7.
He WF, Liang LF, Cai YS, Gao LX, Li YF, Li J, et al. Brominated polyunsaturated lipids with protein tyrosine phosphatase-1B inhibitory activity from Chinese marine sponge Xestospongia testudinaria. J Asian Nat Prod Res. 2015;17:861–6.
Yang M, Liang LF, Wang T, Wang HY, Liu HL, Guo YW. Further brominated polyacetylenes with pancreatic lipase inhibitory activity from Chinese marine sponge Xestospongia testudinaria. J Asian Nat Prod Res. 2017;19:732–7.
He WF, Xue DQ, Yao LG, Li J, Liu HL, Guo YW. A new bioactive steroidal ketone from the South China Sea sponge Xestospongia testudinaria. J Asian Nat Prod Res. 2016;18:195–9.
Sun JZ, Jiang CS, Chen XQ, Chen KS, Zhen XC, Soest RWM. et al. Topsendines A–F, new 3-alkylpyridine alkaloids from a Hainan sponge Topsentia sp. Tetrahedron. 2014;70:3166–71.
Xue DQ, Liu HL, Chen SH, Mollo E, Gavagnin M, Li J, et al. 5-Alkylpyrrole-2-carboxaldehyde derivatives from the Chinese sponge Mycale lissochela and their PTP1B inhibitory activities. Chin Chem Lett. 2017;28:1190–3.
Liu HL, Xue DQ, Chen SH, Li XW, Guo YW. New highly oxidized formamidobisabolene-derived sesquiterpenes from a Hainan sponge Axinyssa variabilis. Helv Chim Acta. 2016;99:650–3.
Li XW, Chen SH, Ye F, Mollo E, Zhu WL, Liu HL, et al. Axiriabilines A–D, uncommon nitrogenous eudesmane-type sesquiterpenes from the Hainan sponge Axinyssa variabilis. Tetrahedron. 2017;73:5239–43.
Han GY, Sun DY, Liang LF, Yao LG, Chen KX, Guo YW. Spongian diterpenes from Chinese marine sponge Spongia officinalis. Fitoterapia. 2018;127:159–65.
Sun DY, Han GY, Yang NN, Lan LF, Li XW, Guo YW. Racemic trinorsesquiterpenoids from the Beihai sponge Spongia officinalis: structure and biomimetic total synthesis. Org Chem Front. 2018;5:1022–7.
Chen B, Gu YC, Voogd NJ, Wang CY, Guo YW. Xidaosterols A and B, two new steroids with unusual α-keto-enol functionality from the South China Sea sponge Neopetrosia chaliniformis. Nat Prod Res. 2022;36:1941–7.
Chen B, Huan XJ, Miao ZH, Voogd NJ, Gu YC, Wang CY, et al. Uncommon bis‐quinolizidine alkaloids from the Hainan sponge Neopetrosia chaliniformis. Chin J Chem. 2021;39:1838–42.
Chen B, Li WS, Gu YC, Zhang HY, Luo H, Wang CY, et al. New sterols from the South China Sea sponges Halichondria sp. Fitoterapia. 2021;152:104918.
Chen B, Li WS, Gu YC, Zhang HY, Luo H, Wang CY, et al. New formamidobisabolene-type sesquiterpenoids from a Hainan sponge Halichondria sp. Tetrahedron. 2021;96:132396.
Chen B, Zhao Q, Gu YC, Lan L, Wang CY, Guo YW. Xishaeleganins A–D, sesquiterpenoid hydroquinones from Xisha marine sponge Dactylospongia elegans. Mar Drugs. 2022;20:118.
Ye F, Zhou YB, Li J, Gu YC, Guo YW, Li XW. New steroids from the South China Sea soft coral Lobophytum sp. Chem Biodivers. 2020;17:e2000214.
Zhang Q, Liang LF, Miao ZH, Wu B, Guo YW. Cytotoxic polyhydroxylated steroids from the South China Sea soft coral Lobophytum sp. Steroids. 2019;141:76–80.
Zhang Q, Li XW, Yao LG, Wu B, Guo YW. Three new capnosane-type diterpenoids from the South China Sea soft coral Lobophytum sp. Fitoterapia. 2019;133:70–4.
Li SW, Cuadrado C, Huan XJ, Yao LG, Miao ZH, Hernandez Daranas A, et al. Rare new bicyclic cembranoid ethers and a novel trihydroxy prenylated guaiane from the Xisha soft coral Lobophytum sp. Bioorg Chem. 2020;103:104223.
Li SW, Cuadrado C, Yao LG, Daranas AH, Guo YW. Quantum mechanical-NMR-aided configuration and conformation of two unreported macrocycles isolated from the Soft Coral Lobophytum sp.: energy calculations versus coupling constants. Org Lett. 2020;22:4093–6.
Yin FZ, Huan XJ, Mudianta IW, Miao ZH, Wang H, Guo YW, et al. Polyoxygenated cembranoids from soft coral Lobophytum Crassum and their anti‐tumoral activities. Chin J Chem. 2021;39:640–6.
Yin FZ, Yao LG, Zhang ZY, Wang JR, Wang H, Guo YW. Polyoxygenated cembranoids from the Hainan soft coral Lobophytum crassum. Tetrahedron. 2021;90:132204.
Cai YS, Cui WX, Tang W, Guo YW. Uncommon terpenoids with anti-inflammatory activity from the Hainan soft coral Sinularia tumulosa. Bioorg Chem. 2020;104:104167.
Chen ZH, Yao LG, Wu Q, Guo YW. Uncommon polycyclic merosesquiterpenoids and asteriscanoids from the Hainan soft coral Sinularia humesi. Chin J Chem. 2021;39:2377–85.
Lu SQ, Li XW, Li SW, Cui Z, Guo YW, Han GY. Sinuhirtins A and B, two uncommon norhumulene-type terpenoids from the South China Sea soft coral Sinularia hirta. Tetrahedron Lett. 2019;60:151308.
Chen WT, Li J, Wang JR, Li XW, Guo YW. Structural diversity of terpenoids in the soft coral Sinularia flexibilis, evidenced by a collection from the South China Sea. RSC Adv. 2015;5:23973–80.
Wu Q, Li XW, Li H, Yao LG, Tang W, Miao ZH, et al. Bioactive polyoxygenated cembranoids from a novel Hainan chemotype of the soft coral Sinularia flexibilis. Bioorg Med Chem Lett. 2019;29:185–8.
Chen ZH, Li WS, Zhang ZY, Luo H, Wang JR, Zhang HY, et al. Sinusiaetone A, an anti-inflammatory norditerpenoid with a bicyclo[11.3.0]hexadecane nucleus from the Hainan soft coral Sinularia siaesensis. Org Lett. 2021;23:5621–5.
Jiang CS, Ru T, Yao LG, Miao ZH, Guo YW. Four new cembranoids from the Chinese soft coral Sinularia sp. and their anti-Aβ aggregation activities. Fitoterapia. 2019;136:104176.
Wu MJ, Wang H, Jiang CS, Guo YW. New cembrane-type diterpenoids from the South China Sea soft coral Sinularia crassa and their α-glucosidase inhibitory activity. Bioorg Chem. 2020;104:104281.
Yang M, Li H, Zhang Q, Wu QH, Li G, Chen KX, et al. Highly diverse cembranoids from the South China Sea soft coral Sinularia scabra as a new class of potential immunosuppressive agents. Bioorg Med Chem. 2019;27:3469–76.
Cui WX, Yang M, Li H, Li SW, Yao LG, Li G, et al. Polycyclic furanobutenolide-derived norditerpenoids from the South China Sea soft corals Sinularia scabra and Sinularia polydactyla with immunosuppressive activity. Bioorg Chem. 2020;94:103350.
Lin N, Wang H, Guo YW. Iso-ximaonanolobatin G, a minor new cembrane-type diterpenoid from the South China Sea soft coral Sinularia nanolobata. J Asian Nat Prod Res. 2022;24:589–95.
Lin N, Li H, Wang JR, Tang W, Zheng MY, Wang H, et al. New cembrane‐type diterpenoids from the South China Sea soft coral Sinularia nanolobata. Chin J Chem. 2022;40:28–38.
Sun LL, Li WS, Li J, Zhang HY, Yao LG, Luo H, et al. Uncommon diterpenoids from the South China Sea soft coral Sinularia humilis and their stereochemistry. J Org Chem. 2021;86:3367–76.
Liu J, Li H, Wu MJ, Tang W, Wang JR, Gu YC, et al. Sinueretone A, a diterpenoid with unprecedented tricyclo[12.1.0.0(5,9)]pentadecane carbon scaffold from the South China Sea soft coral Sinularia erecta. J Org Chem. 2021;86:10975–81.
Liu J, Wu MJ, Li H, Wang H, Tang W, Gu YC, et al. Unusual polyoxygenated casbane diterpenoids from the South China Sea soft coral Sinularia erecta. Bioorg Chem. 2021;114:105028.
Wu MJ, Liu J, Wang JR, Zhang J, Wang H, Jiang CS, et al. Sinucrassins A–K, casbane‐type diterpenoids from the South China Sea soft coral Sinularia crassa. Chin J Chem. 2021;39:2367–76.
Zeng ZR, Li WS, Nay B, Hu P, Zhang HY, Wang H, et al. Sinunanolobatone A, an anti-inflammatory diterpenoid with bicyclo[13.1.0]pentadecane carbon scaffold, and related casbanes from the Sanya Soft Coral Sinularia nanolobata. Org Lett. 2021;23:7575–9.
Robinson DR, West CA. Biosynthesis of cyclic diterpenes in extracts from seedlings of Ricinus communis L. II. conversion of geranylgeranyl pyrophosphate into diterpene hydrocarbons and partial purification of the cyclization enzymes. Biochemistry. 1970;9:80–9.
Sun LL, Li XW, Guo YW. Ximaoornatins A–C, polyoxygenated diterpenoids from the Hainan soft coral Sinularia ornata. Mar Drugs. 2022;20:218.
Li J, Huan XJ, Wu MJ, Chen ZH, Chen B, Miao ZH, et al. Chemical constituents from the South China sea soft coral Sinularia humilis. Nat Prod Res. 2022;36:3324–30.
Ye F, Zhu ZD, Gu YC, Li J, Zhu WL, Guo YW. Further new diterpenoids as PTP1B inhibitors from the Xisha soft coral Sinularia polydactyla. Mar Drugs. 2018;16:103.
Ye F, Chen ZH, Gu YC, Guo YW, Li XW. New lobane-type diterpenoids from the Xisha soft coral Sinularia polydactyla. Chin J Nat Med. 2020;18:839–43.
Ye F, Zhu ZD, Chen JS, Li J, Gu YC, Zhu WL, et al. Xishacorenes A–C, diterpenes with bicyclo[3.3.1]nonane nucleus from the Xisha soft coral Sinularia polydactyla. Org Lett. 2017;19:4183–6.
Kerschgens I, Rovira AR, Sarpong R. Total synthesis of (-)-xishacorene B from (R)-carvone using a C-C activation strategy. J Am Chem Soc. 2018;140:9810–3.
Rovira AR, Muller N, Deng W, Ndubaku C, Sarpong R. Bio-inspired synthesis of xishacorenes A, B, and C, and a new congener from fuscol. Chem Sci. 2019;10:7788–91.
Jones KE, Park B, Doering NA, Baik MH, Sarpong R. Rearrangements of the chrysanthenol core: application to a formal synthesis of Xishacorene B. J Am Chem Soc. 2021;143:20482–90.
Lusi RF, Perea MA, Sarpong R. C-C bond cleavage of α-Pinene derivatives prepared from carvone as a general strategy for complex molecule synthesis. Acc Chem Res. 2022;55:746–58.
Liang LF, Wang XJ, Zhang HY, Liu HL, Li J, Lan LF, et al. Bioactive polyhydroxylated steroids from the Hainan soft coral Sinularia depressa Tixier-Durivault. Bioorg Med Chem Lett. 2013;23:1334–7.
Yang M, Cui WX, Li H, Li SW, Yao LG, Tang W, et al. Sinulasterols A–C, three new bioactive oxygenated steroids from the South China Sea soft coral Sinularia depressa. Steroids. 2020;157:108598.
Chen WT, Liu HL, Yao LG, Guo YW. 9,11-Secosteroids and polyhydroxylated steroids from two South China Sea soft corals Sarcophyton trocheliophorum and Sinularia flexibilis. Steroids. 2014;92:56–61.
Jiang CS, Ru T, Huan XJ, Miao ZH, Guo YW. New cytotoxic ergostane-type sterols from the Chinese soft coral Sinularia sp. Steroids. 2019;149:108425.
Yang M, Liang LF, Li H, Tang W, Guo YW. A new 5α,8α-epidioxysterol with immunosuppressive activity from the South China Sea soft coral Sinularia sp. Nat Prod Res. 2020;34:1814–9.
Li SW, Chen WT, Yao LG, Guo YW. Two new cytotoxic steroids from the Chinese soft coral Sinularia sp. Steroids. 2018;136:17–21.
Liu J, Wu X, Yang M, Gu YC, Yao LG, Huan XJ, et al. Erectsterates A and B, a pair of novel highly degraded steroid derivatives from the South China Sea soft coral Sinularia erecta. Steroids. 2020;161:108681.
Jia R, Kurtan T, Mandi A, Yan XH, Zhang W, Guo YW. Biscembranoids formed from an α,β-unsaturated γ-lactone ring as a dienophile: structure revision and establishment of their absolute configurations using theoretical calculations of electronic circular dichroism spectra. J Org Chem. 2013;78:3113–9.
Li YF, He LL, Liu HL, Liang LF, Zhang HB, Guo YW. Structural revision of methyl tortuoate D, a bis-cembranoid from Hainan Sarcophyton tortuosum and its absolute stereochemistry. J Asian Nat Prod Res. 2013;15:566–73.
Li Y, Li S, Cuadrado C, Gao C, Wu Q, Li X, et al. Polyoxygenated anti-inflammatory biscembranoids from the soft coral Sarcophyton tortuosum and their stereochemistry. Chin Chem Lett. 2021;32:271–6.
Liang LF, Lan LF, Taglialatela-Scafati O, Guo YW. Sartrolides A–G and bissartrolide, new cembranolides from the South China Sea soft coral Sarcophyton trocheliophorum Marenzeller. Tetrahedron. 2013;69:7381–6.
Liang LF, Gao LX, Li J, Taglialatela-Scafati O, Guo YW. Cembrane diterpenoids from the soft coral Sarcophyton trocheliophorum Marenzeller as a new class of PTP1B inhibitors. Bioorg Med Chem. 2013;21:5076–80.
Liang LF, Kurtan T, Mandi A, Yao LG, Li J, Zhang W, et al. Unprecedented diterpenoids as a PTP1B inhibitor from the Hainan soft coral Sarcophyton trocheliophorum Marenzeller. Org Lett. 2013;15:274–7.
Liang LF, Kurtán T, Mándi A, Gao LX, Li J, Zhang W, et al. Sarsolenane and capnosane diterpenes from the Hainan soft coral Sarcophyton trocheliophorum Marenzeller as PTP1B Inhibitors. Eur J Org Chem. 2014;2014:1841–7.
Yao LG, Zhang HY, Liang LF, Guo XJ, Mao SC, Guo YW, Yalongenes A. and B, two new cembranoids with cytoprotective effects from the Hainan soft coral Sarcophyton trocheliophorum Marenzeller. Helv Chim Acta. 2012;95:235–9.
Chen WT, Yao LG, Li XW, Guo YW. Sarcophytrols A–C, new capnosane diterpenoids from the South China Sea soft coral Sarcophyton trocheliophorum. Tetrahedron Lett. 2015;56:1348–52.
Chen WT, Liang LF, Li XW, Xiao W, Guo YW. Further new highly oxidative cembranoids from the Hainan soft coral Sarcophyton trocheliophorum. Nat Prod Bioprospect. 2016;6:97–102.
Liang LF, Chen WT, Li XW, Wang HY, Guo YW. New bicyclic cembranoids from the South China Sea soft coral Sarcophyton trocheliophorum. Sci Rep. 2017;7:46584.
Liang LF, Chen WT, Mollo E, Yao LG, Wang HY, Xiao W, et al. Sarcophytrols G–L, novel minor metabolic components from South China Sea soft coral Sarcophyton trocheliophorum Marenzeller. Chem Biodivers. 2017;14:e1700079.
Liang LF, Kurtán T, Mándi A, Yao LG, Li J, Lan LF. et al. Structural, stereochemical, and bioactive studies of cembranoids from Chinese soft coral Sarcophyton trocheliophorum. Tetrahedron. 2018;74:1933–41.
Chen ZH, Gao TR, Yang M, Yao LG, Guo YW. Further new cembranoids from the South China Sea soft coral Sarcophyton trocheliophorum. Fitoterapia. 2021;151:104902.
Li G, Li H, Zhang Q, Yang M, Gu YC, Liang LF, et al. Rare cembranoids from Chinese soft coral Sarcophyton ehrenbergi: structural and stereochemical studies. J Org Chem. 2019;84:5091–8.
Li G, Li H, Tang W, Yao LG, Liang LF, Guo YW. Further polyoxygenated cembranoids from South China Sea soft coral Sarcophyton ehrenbergi. Bioorg Chem. 2020;101:103993.
Shen SM, Li WS, Ding X, Luo H, Zhang HY, Guo YW. Ximaoglaucumins A–F, new cembranoids with anti-inflammatory activities from the South China Sea soft coral Sarcophyton glaucum. Bioorg Med Chem. 2021;38:116139.
Ye F, Gu YC, Guo YW, Li XW. Absolute configurations of new cembrane-type diterpenoids from the Hainan soft coral Sarcophyton crassocaule. Tetrahedron Lett. 2020;61:152008.
Yang M, Li XL, Wang JR, Lei X, Tang W, Li XW, et al. Sarcomililate A, an unusual diterpenoid with tricyclo[11.3.0.0(2,16)]hexadecane carbon skeleton, and its potential biogenetic precursors from the Hainan soft coral Sarcophyton mililatensis. J Org Chem. 2019;84:2568–76.
Ye F, Li J, Wu Y, Zhu ZD, Mollo E, Gavagnin M, et al. Sarinfacetamides A and B, nitrogenous diterpenoids with tricyclo[6.3.1.0(1,5)]dodecane scaffold from the South China Sea soft coral Sarcophyton infundibuliforme. Org Lett. 2018;20:2637–40.
Yang F, Li SW, Zhang J, Liang LF, Lu YH, Guo YW. Uncommon nornardosinane, seconeolemnane and related sesquiterpenoids from Xisha soft coral Litophyton nigrum. Bioorg Chem. 2020;96:103636.
Yang F, Hua Q, Yao LG, Liang LF, Lu YH, An FL, et al. Further new nardosinane-type sesquiterpenoids from the Xisha soft coral Litophyton nigrum. Fitoterapia. 2021;151:104906.
Yang F, Hua Q, Yao LG, Liang LF, Lou YX, Lu YH, et al. One uncommon bis-sesquiterpenoid from Xisha soft coral Litophyton nigrum. Tetrahedron Lett. 2022;88:153571.
Wu Q, Li H, Yang M, Jia AQ, Tang W, Wang H, et al. Two new cembrane-type diterpenoids from the Xisha soft coral Lemnalia flava. Fitoterapia. 2019;134:481–4.
Wu Q, Ye F, Li XL, Liang LF, Sun J, Sun H, et al. Uncommon polyoxygenated sesquiterpenoids from South China Sea soft coral Lemnalia flava. J Org Chem. 2019;84:3083–92.
Gao Y, Xiao W, Liu HC, Wang JR, Yao LG, Ouyang PK, et al. Clavuridins A and B, two new trinor-guaiane sesquiterpenes isolated from the Xisha soft coral Clavularia viridis. Chin J Nat Med. 2017;15:855–9.
Wu Q, Gao Y, Zhang MM, Sheng L, Li J, Li XW, et al. New sesquiterpenoids from the South China Sea soft corals Clavularia viridis and Lemnalia flava. Beilstein J Org Chem. 2019;15:695–702.
Gao Y, Xiao W, Liu HC, Wang JR, Yao LG, Ouyang PK, et al. Clavirolide G, a new rare dolabellane-type diterpenoid from the Xisha soft coral Clavularia viridis. Chin Chem Lett. 2017;28:905–8.
Gao Y, Du YQ, Zang Y, Liu HC, Wan HY, Li J, et al. Dolabellane diterpenoids from the Xisha soft coral Clavularia viridis. ACS Omega. 2022;7:3052–9.
Ru T, Cai YS, Li H, Tang W, Wang H, Guo YW. Further new eunicellin-based diterpenoids from the Guangxi Weizhou soft coral Cladiella krempfi. Fitoterapia. 2018;131:200–3.
Cai YS, Yao LG, Di Pascale A, Irace C, Mollo E, Taglialatela-Scafati O, et al. Polyoxygenated diterpenoids of the eunicellin-type from the Chinese soft coral Cladiella krempfi. Tetrahedron. 2013;69:2214–9.
Li G, Sun LL, Dickschat JS, Guo YW. Klyflaccilins B–T, polyoxgenated eunicellins from the soft coral Klyxum flaccidum. Eur J Org Chem. 2021;2021:1402–6.
Li G, Li H, Tang W, Guo YW, Li XW. Klyflaccilides A and B, diterpenoids with 6/5/8/3 fused tetracyclic carbon skeleton from the Hainan soft coral Klyxum flaccidum. Org Lett. 2019;21:5660–4.
Huang RY, Chen WT, Kurtan T, Mandi A, Ding J, Li J, et al. Bioactive isoquinolinequinone alkaloids from the South China Sea nudibranch Jorunna funebris and its sponge-prey Xestospongia sp. Future Med Chem. 2016;8:17–27.
Wu Q, Li SW, Voogd NJ, Wang H, Yao LG, Guo YW, et al. Marine alkaloids as the chemical marker for the prey-predator relationship of the sponge Xestospongia sp. and the nudibranch Jorunna funebris. Mar Life Sci Technol. 2021;3:375–81.
He WF, Li Y, Feng MT, Gavagnin M, Mollo E, Mao SC, et al. New isoquinolinequinone alkaloids from the South China Sea nudibranch Jorunna funebris and its possible sponge-prey Xestospongia sp. Fitoterapia. 2014;96:109–14.
Wu Q, Chen WT, Li SW, Ye JY, Huan XJ, Gavagnin M, et al. Cytotoxic nitrogenous terpenoids from two South China Sea nudibranchs Phyllidiella pustulosa, Phyllidia coelestis, and their sponge-prey Acanthella cavernosa. Mar Drugs. 2019;17:56.
Shen SM, Zhang ZY, Yao LG, Wang JR, Guo YW, Li XW. Nitrogenous sesquiterpenoids from the South China Sea nudibranch Hexabranchus sanguineus and its possible sponge‐prey Acanthella cavernosa: chiral Separation, stereochemistry and chemical ecology. Chin J Chem. 2021;40:235–46.
Li XL, Li SW, Yao LG, Mollo E, Gavagnin M, Guo YW. The chemical and chemo-ecological studies on Weizhou nudibranch Glossodoris atromarginata. Magn Reson Chem. 2021;59:554–60.
Wu Q, Li SW, Xu H, Wang H, Hu P, Zhang H, et al. Complex polypropionates from a South China Sea photosynthetic mollusk: isolation and biomimetic synthesis highlighting novel rearrangements. Angew Chem Int Ed Engl. 2020;59:12105–12.
Zhou ZF, Li XL, Yao LG, Li J, Gavagnin M, Guo YW. Marine bis-γ-pyrone polypropionates of onchidione family and their effects on the XBP1 gene expression. Bioorg Med Chem Lett. 2018;28:1093–6.
Li SW, Cui WX, Huan XJ, Gavagnin M, Mollo E, Miao ZH, et al. A new bis-γ-pyrone polypropionate of onchidiol family from marine pulmonate mollusk Onchidium sp. Nat Prod Res. 2020;34:1971–6.
Acknowledgements
The authors wish to acknowledge all of their colleagues who have contributed to the studies presented herein. The reported researches were financially supported by the National Natural Science Foundation of China (No 81991521), the SKLDR/SIMM Project (No. SIMM2103ZZ‐06), and Syngenta-SIMM-PhD Studentship Project.
Author information
Authors and Affiliations
Corresponding authors
Ethics declarations
Competing interests
The authors declare no competing interests.
Supplementary information
Rights and permissions
Springer Nature or its licensor holds exclusive rights to this article under a publishing agreement with the author(s) or other rightsholder(s); author self-archiving of the accepted manuscript version of this article is solely governed by the terms of such publishing agreement and applicable law.
About this article
Cite this article
Liu, J., Gu, Yc., Su, Mz. et al. Chemistry and bioactivity of secondary metabolites from South China Sea marine fauna and flora: recent research advances and perspective. Acta Pharmacol Sin 43, 3062–3079 (2022). https://doi.org/10.1038/s41401-022-00980-w
Received:
Accepted:
Published:
Issue Date:
DOI: https://doi.org/10.1038/s41401-022-00980-w
Keywords
This article is cited by
-
APS celebrates the 90th anniversary of SIMM
Acta Pharmacologica Sinica (2022)
