Normal eye colour and pigmentation of the iris

The anatomy of iris pigmentation

Anatomically the iris is composed of two layers of different embryological origin. The anterior layer is the iris stroma, which is derived from the mesoderm and consists of a loose collagenous network, which contains the sphincter pupillae muscle, blood vessels, nerves, and cellular elements, including fibroblasts, melanocytes, clump cells, and mast cells. The anterior border layer is a condensation of connective tissue of the anterior stroma and contains numerous pigment cells. Iris stromal, ciliary body, and choroidal melanocytes are all derived from the neural crest, a transient population of cells, unique to vertebrates.1, 2 Uveal melanocytes differ from their cutaneous counterparts in one important respect: cutaneous melanocytes ‘inoculate’ melanosomes into the surrounding epithelial cells; by contrast, uveal melanocytes remain continent and do not release melanosomes into the surrounding tissues. The posterior pigment epithelium forms the posterior layer and is neuroectodermal in origin. The posterior pigment epithelium is derived from the anterior portion of the optic cup. It consists of two layers of cuboidal pigment cells, which are tightly joined to each other by numerous intercellular junctions.1, 2

It is believed that there are four main factors, which determine iris colour: the pigment granules within the posterior pigment epithelium, the concentration of pigment within the iris stromal melanocytes, the nature of melanin pigment within the iris melanocytes, and the light-scattering and absorption properties of the extracellular stromal matrix.3, 4 It is generally considered that the concentration of melanosomes in the posterior pigment epithelium is relatively constant in normal individuals and as a result it has little impact differences in normal eye colour. The posterior pigment epithelium is only an important determinant of eye colour when it is deficient in normal melanosomes in conditions such as albinism.

The density of the iris stroma is the main determinant of colour in blue irides. The blue appearance is a result of backscatter of incident light by stromal collagen fibres. Light of longer wavelength readily penetrates the iris and is absorbed, whereas light with a shorter wavelength is reflected back and scattered by the stromal matrix.2, 3 The pigment content of the iris stroma and anterior border layer is responsible for determining all of the shades of iris colour from green to dark brown. Increasing pigment within the iris stroma leads to greater light absorption and the resulting darker eye colour.3 While increasing stromal pigment content undoubtedly influences iris colour, some controversy still remains as to whether this is due to an increased number of pigment cells, the density of pigment within the cells (melanosome density in size), or the type of melanin contained within the melanosome. Although studies by Fuchs5 and Dietrich6 supported the notion that the number of melanocytes in the anterior border layer accounted for the differences in iris colour, other studies have concluded that the number of melanocytes within the anterior border layer are relatively constant, irrespective of eye colour.7 Further studies using electron microscopy and immunohistochemistry to examine the morphology and quantity of stromal melanocytes have again concluded that the relative numbers of these cells is not a major determinant to iris colour.3, 8, 9 It would appear based on the electron microscopy of the iris stroma that the number and size of melanosomes contained within melanocytes may have a significant role in determining eye colour.8, 9

Melanin is an inert biopolymer that exists in two distinct forms: brown-black eumelanin and red-yellow pheomelanin. Melanocytes have the capacity to produce both forms of melanin; however, the ratio of the two forms can vary widely in individuals, producing different shades of hair and skin colour.10 In a recent study Prota et al4 characterised the type of melanin, which occurred in human irides. They concluded that the melanocytes within the posterior pigment epithelium contained essentially eumelanin, whereas those extracted from iris tissue in which the pigment epithelium had been removed by scraping (consisting of mainly stroma and anterior iris pigment epithelium (IPE)) contained both eumelanin and pheomelanin. Furthermore, they noted that pheomelaninic-type pigmentation was associated with green irides, whereas green blue mixed colour irides contained mostly eumelanin. By contrast, they were unable to categorise green-brown or brown irides into either of the two forms and concluded that they probably contained mixed pigment content.

The final adult iris colour is not present at birth, and in Caucasians the neonatal iris is blue as a result of a paucity of stromal melanocytes, which, presumably, have yet to migrate from the neural crest or differentiate from the primitive precursor cells. In non-White races the iris appears slate grey at birth. The iris normally adopts its true adult colour by the age of 3–5 months.1

The genetics of eye colour

In the first decade of the 20th century two reports appeared in the literature, which supported the notion that eye colour was inherited as a simple Mendelian trait.11, 12 Brown eye colour was inherited as a dominant trait and blue eye colour as a recessive one, and, as a result, two blue-eyed parents were incapable of producing children with brown eyes. Although this doctrine was widely taught, it soon became apparent that occasionally blue-eyed parents could produce brown-eyed offspring and that eye colour was not inherited as a simple Mendelian trait.13 Indeed, recent studies suggest that eye colour is inherited as a polygenic trait, which, as yet, is incompletely understood.

A number of pigment genes have been implicated in determining eye colour: these include OCA2, TYRP1, MAPT, and MYO5A.10 Of these, the OCA2 gene, which is located in the long arm of chromosome-15 (15q11.2–15q-12) would appear to be the most influential.14 Mutation of OCA2 is the underlying cause of oculocutaneous albinism type-II. Moreover, deletion of the region encompassing this gene on chromosome-15 has been associated with the hypo-pigmentation of hair, skin, and eyes found in the Angelman and Prader–Willi syndromes.15 Duffy et al15 have recently reported that a Three-Single-Nucleotide polymorphism haplotype in intron-1 of the OCA2 gene can explain most of the variation in human eye colour.

Congenital anomalies and abnormalities of iris pigmentation

Binocular and sectorial heterochromia

Although, as we shall see later, both binocular and sectorial heterochromia are frequently associated with pathological conditions affecting the iris, they may, on occasion, arise as an isolated congenital abnormality.16 Sectorial heterochromia (heterochromia iridis) arises when areas of the same iris are different in colour. This condition may be unilateral or bilateral. Several reports in the early literature suggests that this condition may arise as an autosomal dominant trait.16 It remains uncertain as to whether any of these early reports were in fact describing patients with Waardenburg syndrome. Moreover, sectorial heterochromia may be confused with an extensive iris naevus. Recently, bilateral sectorial iris heterochromia has been described in a case of chromosome 13q deletion syndrome.17

Binocular heterochromia (heterochromia iridum) has been recognised, in both humans and animals, from the very early times and was referred to as ‘heteroglaucos’ by Aristotle.16 The Byzantine Emperor Anastasius I was called Dicorous because, according to chroniclers, his right eye was ‘glauci’ (bluish green or bluish grey) and the left eye black. Both eyes were apparently normal in all other respects. Anastasius I was over 90 years old when he died and this would suggest that he was not suffering from any systemic disease or syndrome, which would have normally foreshortened his lifespan.18 According to Plutarch, Alexander the Great also suffered from heterochromia iridum.16 Binocular heterochromia may arise as an isolated congenital anomaly or as an autosomal dominant trait.16 Heterochromia iridum has also been reported in association with Sturge–Weber syndrome,19 hypomelanosis of Ito,20 and linear scleroderma.21 Recently, Quinlan and Shwayder22 reported a case of a large facial café au lait macule in association with heterochromia iridum. The macule was extensive and involved both the upper and the lower eyelids. The patient had one blue and one brown iris. Interestingly, the blue iris was on the same side as the café au lait macule. Heterochromia has also been described in association with iris colobomas. In a study of 75 children in Scotland with iris colobomas, 13 (17.3%) of these patients were noted to be suffering from iris heterochromia. In cases where the coloboma was unilateral, the affected iris was always darker in colour.23

Congenital Horner's syndrome

In 1893 Angelucci noted a de-pigmentation of the uveal tract of dogs and rabbits, which had been subjected to surgical excision of the superior cervical ganglion,16 and in 1904 Abelsdorff24 noted heterochromia in cats following similar procedures. Subsequently, Calhoun in 191925 reported a series of experiments on rabbits and rodents in which he noted that hypo-pigmentation of the iris was related to the length of survival after sympathectomy. Clinically, the association of congenital Horner's syndrome and iris de-pigmentation, producing heterochromia, is well-recognised. Weinstein et al26 found iris heterochromia in 9 of 11 patients with congenital Horner's syndrome and in all cases the site of the lesion was considered to be due to disruption of the postganglionic neurone. In one of the remaining patients, both irides were very light blue, making the diagnosis of heterochromia impossible. The final patient did not suffer from heterochromia and was considered to have an interruption of the pre-ganglionic pathway. They considered that disruption of the postganglionic pathway could lead to a neurotropic dysgenesis of iris melanocytes.26 In a further study of 23 children presenting with Horner's syndrome in the first year of life, 78% were found to have iris heterochromia.27

Although less common, it would appear that cases of acquired Horner's syndrome in childhood and adult life may occasionally also give rise to iris heterochromia. Laties28 reported a case of a 29-year-old female who had developed Horner's syndrome, with associated heterochromia, following the removal of a neurolemmoma when aged 14. Diesenhouse et al29 subsequently reported two cases of Horner's syndrome following sympathectomy, which were associated with the development of iris hypo-pigmentation. A number of reports in the literature have also indicated the development of iris heterochromia in children who develop Horner's syndrome as a result of either a cervical ganglioneuroma,30 neurolemmoma,31 or neuroblastoma.32, 33 Again, it is interesting to note that in all cases of heterochromia-associated acquired Horner's syndrome, the causal lesion was postganglionic in origin.

The development of iris hypo-pigmentation following disruption to the postganglionic sympathetic fibres to the eye clearly suggests that adrenergic innervation is important in the maintenance of iris pigmentation. Laties28 in a study of the effect of sympathectomy in rabbits, noted a rapid reduction in tyrosinase activity in both the iris and the choroid following interruption to the sympathetic innervation of the eye. Furthermore, Mukuno and Witmer34 in an electron microscopic study of the human iris, identified contacts between melanocytes and nerve terminals in the stroma. They described four distinct types of nerve terminals apparently making synaptic contact with melanocytes and concluded that at least two of these were adrenergic in origin. Adrenergic innervation of melanocytes has also been reported in the iris of monkeys and rabbits.35 McCartney et al36 undertook an electron microscopic study of an iris in a case of congenital Horner's syndrome. They noted a significant reduction in melanocytes in both the anterior border and stromal layers when compared with the unaffected iris. The number of melanosomes in the residual melanocytes did not appear to be reduced. The authors concluded that the reduction in melanocytes in the anterior border and stromal layers may have been due to failure of migration of neural crest-derived melanocytes in the early postnatal period. Iris hypo-pigmentation in cases of Horner's syndrome in adult life could be due to an attrition of the normal monocyte population following sympathetic denervation.36 Interestingly, three naevi were present on the surface of the affected iris and these showed no signs of pigment loss: a finding also noted by Dryja and Albert37 in a clinical study of an affected iris. These findings suggest that naevus cells do not share the same sympathetic innervation as stromal melanocytes.

Waardenburg syndrome

In 1947 Waardenburg, a Dutch ophthalmologist and geneticist, described a deaf mute man with medial canthal dystopia, blepharophimosis, and partial iris atrophy to a meeting of the Dutch Ophthalmological Society.38 He noted similarities in this case and those previously described in a pair of monozygotic twin girls.39 Waardenburg subsequently undertook a systematic search among 1050 inmates of five Dutch institutions for the deaf; he found 12 individuals with clinical manifestations of the disease.38, 40 The results of this study were published in a seminal paper in the American Journal of Human Genetics in 195141 and define the syndrome now known as Waardenburg syndrome type-I, which had six main features: lateral displacement of the medial canthi combined with dystopia of the lacrimal punctum and blepharophimosis; prominent broad nasal root; hypertrichosis of the medial part of the eyebrows, white forelock, heterochromia iridis; and deaf-mutism.40, 41 There are now four recognised variants of Waardenburg syndrome (types I–IV) all of which are inherited by an autosomal dominant trait, with the exception of Waardenburg syndrome type-IV, which appears to have a mostly autosomal recessive mode of inheritance.38 Mutations of the PAX3 gene have been implicated in Waardenburg syndrome types I and III, whereas approximately 15% of type-II have mutations of the MITF gene.40 Mutations of the endothelin-3 (EDN3), endothelin receptor-B (EDNRB), and SOX10 genes have been found in patients with Waardenburg syndrome type-IV.40, 42 PAX3, MITF, and SOX10 are transcription factors and EDNRB and EDN3 are signalling molecules, all of which appear to have a role in the development of melanocytes from primitive neural crest cells.43, 44

Three types of pigmentary disturbance of the iris have been observed in Waardenburg syndrome and include complete heterochromia iridis, partial, or segmental heterochromia (Figure 1a), which maybe unilateral or bilateral, and bilateral isohypochromia iridis (pale blue eyes).38, 40 Iris heterochromia, either partial or complete, is found in between 21 and 28% of individuals with Waardenburg syndrome40 and appears to be most common in the type-II variant, with a reported frequency of 47%.45 Isohypochromia iridis has a reported incidence of 14.9–42%.40

Figure 1
figure 1

(a) Sectorial pigmentation in Waardenburg syndrome. (b) Lisch nodules in neurofibromatosis type-I. Note the predominant inferior location. (c) Anterior stromal cyst containing a turbid sediment. (d) Multiple posterior pigment epithelial cysts. This patient presented with raised intraocular pressure. Note the plateaux iris configuration. (e) A large iris metastasis in a patient with an occult bronchiogenic carcinoma. (f) A peripheral iris melanocytoma.

Histopathological studies of the irides of patients with Waardenburg syndrome are limited. Mullaney et al46 described the light and electron microscopic findings of the irides in a patient with the type-II variant of Waardenburg syndrome. They found a reduction in the number of stromal melanocytes in deep blue iris when compared with the fellow brown eye. Furthermore, the melanosomes were smaller and fewer in number in the blue iris when compared with the brown iris.46

Iris freckles

Iris freckles are flat, discrete areas of brown pigmentation on the iris surface. They do not distort the architecture of the iris stroma: an important clinical sign when differentiating them from naevi and other melanocytic tumours of the iris. Iris freckles are extremely common and may be found in over 60% of the general population.47 There is no evidence to suggest that iris freckles are capable of malignant transformation.

Lisch nodules

In 1937 Karl Lisch48 reported his observations of brown nodules on the surface of the iris in three patients with neurofibromatosis and as a result such lesions now bear his name. However, as is the case with many medical eponymous terms, Lisch was not first to describe the presence of pigmented iris nodules in neurofibromatosis. Snell and Treacher Collins,49 Goldstein and Wexler,50 Fuchs,51 and Sakurai52 all describe similar patients prior to Lisch. Moreover, Van der Hoeve53 in his 1932 Doyne Memorial lecture on the eye symptoms in phakomatoses described a family with neurofibromatosis and iris lesions originally observed by Waardenburg. Although not pathognomonic, Lisch nodules rarely occur in patients not suffering from neurofibromatosis type-I. Lal et al54 reported a case of unilateral Lisch nodules in a 14-year-old boy who otherwise had no other signs of NF1. They commented that this could represent a somatic mutation of the NF1 with limited mosaicism, perhaps limited to only that sector of the iris. Lisch nodules have also been described in Cushing's disease,55 familial angiolipomatosis,56 and neurofibromatosis type-II.57

Lisch nodules are not present at birth and usually appear in the late childhood, after the appearance of café au lait spots but before the development of overt neurofibromas.58 Almost all patients with NF1 older than 20 years of age will have Lisch nodules.59 Clinically, Lisch nodules are small (>1 mm diameter) discrete yellow or brown, dome-shaped nodules on the surface of the iris. They usually have a smooth surface with a gelatinous like interior. While the finding of two or more Lisch nodules is one of the diagnostic criteria for NF1, most affected irides contain many more and occasionally in excess of a hundred are found to be present in the adult eye.58

Early histopathological studies suggested that Lisch nodules were melanocytic hamartomas. In 1982 Perry and Font described the electron microscopic appearances of Lisch nodules in an iridectomy specimen obtained from a 75-year-old male suffering from NF1. They found that the nodules were composed of spindle-shaped cells, which were melanocytic in origin, and based on these observations they suggested that they were indeed melanocytic hamartomas.60 Williamson et al61 in a further electron microscopic study also suggested that Lisch nodules were melanocytic in origin. However, more recent observations have cast doubt on the hamartomatous nature of these lesions and suggest that they should be considered as benign iris tumours. Richetta et al62 studied the histopathological and ultrastructural features of a Lisch nodule obtained from a 50-year-old woman with NF1 and found that it was composed of three main cell types: pigmented cells, fibroblast-like cells, and mast cells. They concluded that Lisch nodules were histologically similar to neurofibromas. Clinical studies have also challenged the concept that Lisch nodules are true hamartomas. Nichols et al63 in a study of 369 patients with NF1 noted that in 80% of affected eyes the Lisch nodules were located inferiorly. Wood et al64 reported a single case of inferiorly located Lisch nodules in a patient suffering from bilateral ptosis. In a recent study Boley et al65 mapped and quantified the distribution of Lisch nodules in 73 adults with NF1 and found that the number of nodules in the inferior hemifield was statistically greater when compared with the superior hemifield (Figure 1b). They also noted that the light irides harboured significantly more Lisch nodules than the dark irides. These findings suggest that Lisch nodules may arise secondary to exposure to UV light from sunlight for it is thought that the lower half of the iris receives a greater amount of incident sunlight than the upper hemifield.66, 67 Indeed, as we shall see later, iris melanomas are also usually located in the inferior hemifield. If UV exposure is a factor in the development of Lisch nodules, then this presumably is due to DNA damage, which would suggest that these lesions are benign tumours rather than true hamartomas. Although elements of this argument are persuasive, it does not explain why these lesions are homogeneous in appearance, fail to continue to grow throughout life, and apparently do not undergo occasional malignant transformation as would be expected with other benign tumours.

Ocular/oculodermal melanocytosis

In 1861 Hulke68 reported a case of a uveal malignant melanoma arising in a female patient who was noted to have pigmentation of the eyelid, eyebrow sclera, and fundus. A number of sporadic cases involving pigmentation of the peri-ocular skin, sclera, and conjunctiva subsequently appeared in the literature69 before, in 1938, Ota70 at a meeting of the dermatological society in Japan, described the condition, which now bears his name. The following year Tanino71, Ota's pupil, published a report of 26 cases of Naevus of Ota. Fitzpatrick et al72 first proposed the term oculodermal melanocytosis for Naevus of Ota and ocular melanocytosis for pigmentation of the ocular tissues in the absence of an associated peri-ocular naevus. It is now apparent that these conditions represent a spectrum of congenital pigmentation involving the skin and/or ocular tissues. In a study by Teekhasaenee et al73 of 194 affected patients, they found that 67 (34.5%) had skin involvement alone, 12 (6.2%) had only ocular involvement, and the remaining 115 (59.3%) had both ocular and dermal pigmentation.

Histologically, the cutaneous elements of oculodermal melanocytosis contain spindle and dendritic cells in the dermis resembling melanocytes migrating from the neural crest to the epidermis.74 In this respect oculodermal melanocytosis is similar to Mongolian spot, naevus of Ito, and blue naevus. Histopathological studies of affected eyes have shown the presence of pigmented stellate melanocytes distributed throughout the sclera and episcleral tissues together with increased numbers of benign plump dendritic monocytes within the choroid.75, 76, 77 An ultrastructural study of an affected iris demonstrated the presence of numerous melanocytes in the anterior border and iris stromal layers. Many of these melanocytes, in addition to a normal-sized melanosomes, contained large round macromelanosomes, which probably reflects a basic defect in melanogenesis within the cells.77

Naevus of Ota together with naevus of Ito and Mongolian spot have been classified as hamartomatous congenital dermal melanocytoses involving the migration of neural crest-derived melanocytes during embryogenesis.74 Indeed, it has been suggested that Naevus of Ota arises as a result of an arrest in the migration of neural crest melanocytes, which leads to the aggregation of these cells in the dermis.78 While this hypothesis provides a plausible explanation for the presence of melanocytes within the affected dermis, it does not explain the excessive numbers of melanocytes found within the ocular tissues. Other explanations include local changes in the embryonic environment, which leads to the preferential differentiation of migrating neural crest cells into a melanocytic phenotype.79 Whatever the precise explanation, there can be little doubt that ocular and oculodermal melanocytosis arise as a result of a perturbation of migrating neuro crest melanocytes.

Oculodermal melanocytosis is apparent at or soon after birth; in over 50% of cases it is almost always manifest by the end of the second decade of life.73, 80 Ocular melanocytosis (Naevus of Ota) is more common in Orientals than in Caucasian or Black individuals. Studies in Japan have reported a prevalence ranging from 0.4 to 0.84%.81 In a study to determine the prevalence rate of ocular and oculodermal melanocytosis Gonder et al81 found the prevalence of ocular melanocytosis in White individuals to be 0.038% and oculodermal melanocytosis in the Black population to be 0.014%. Oculodermal melanocytosis is generally considered to occur more frequently in females. Hidano et al80 reported that oculodermal melanocytosis occurred five times more frequently in women than in men. However, other investigators have suggested that this apparent predilection for females may be distorted by the fact that women may be more likely to present to dermatology clinics as a result of their cosmetic appearance than males.73 Oculodermal melanocytosis is usually a unilateral, although sporadic cases of bilateral involvement have been reported in the literature.82, 83, 84, 85, 86, 87, 88 The vast majority of cases of ocular or oculodermal melanocytosis are sporadic in nature and only rarely have familial cases been reported in the literature.89, 90, 91, 92

Clinically, oculodermal melanocytosis is characterised by a bluish-grey pigmentation88 involving areas of skin innervated by the first and the second divisions of the trigeminal nerve. Occasionally, there may be pigmentation of the eardrum, buccal mucosa, palate, nasopharynx, and leptomeninges.78, 93 A number of ocular tissues may be involved, including the conjunctiva, episclera, cornea, iris, lens, anterior chamber angle, choroid, and optic disc.73 The episclera is almost always involved and may range from relatively discreet bluish spots to confluent dark mottled patches, which are dispersed randomly on the globe, but usually do not involve the limbus.73 Episcleral blood vessels crossing the involved areas are frequently separated from the pigmentation by a narrow, non-pigmented band. Hyper-pigmentation of the choroid producing a dark fundus when compared with the fellow eye is found in approximately 80% of cases.73 Iris involvement, which may be generalised or sectorial, is present in almost 90% of cases. The degree of iris involvement is variable and ranges from the presence of stellate granules on an otherwise normal iris to a dense uniform pigmentation, which obscures the underlying iris architecture.73 Iris mammillations, which appear as regularly spaced, deep brown, smooth, conical elevations that cover the iris surface giving it a velvety appearance to the naked eye, are found in cases of ocular and oculodermal melanocytosis.94 These changes may be the initial manifestation of ocular melanocytosis in the absence of conjunctival or episcleral pigmentation.95 Iris mammillations are not exclusive to ocular melanocytosis and have been observed sporadically or in association with systemic conditions, including phakomatosis pigmentovascularis type-IIb and neurofibromatosis type-I.94 Rarely, iris mammillations may be familial.96

Ocular and oculodermal melanocytosis have been reported in association with a number of ocular conditions, including; glaucoma,73, 97, 98, 99, 100, 101, 102, 103 retinitis pigmentosa,104 congenital cataract,105 and Duane's syndrome.106 However, there can be little doubt that the most important association is the development of uveal melanoma in the eyes involved by these conditions. There have been numerous reports in the literature since the first description by Hulke68 of the development of uveal melanomas in cases of ocular and oculodermal melanocytosis.75, 76, 86, 95, 107, 108, 109, 110, 111, 112, 113, 114, 115, 116, 117, 118, 119, 120, 121, 122, 123, 124, 125, 126, 127, 128, 129, 130, 131, 132, 133, 134, 135 Singh et al136 estimated the lifetime risk of a patient with ocular or oculodermal melanocytosis of developing a uveal melanoma to be approximately 1 in 400 as compared with 1 in 13 000 for the general population. This represents an approximately 30-fold increased risk. Ninety percent of the patients who developed a melanoma did so between the ages of 31 and 80 years. There have been relatively few reports of iris melanomas developing in the context of ocular or oculodermal melanocytosis, which probably reflects a relative rarity of these tumours when compared with posterior uveal melanomas.113, 132, 134, 135

Iris cysts

Primary iris stromal cysts

Primary iris stromal cysts are rare, with the majority of reports in the literature limited to single case studies.137, 138, 139, 140, 141, 142, 143, 144, 145, 146, 147, 148, 149, 150, 151, 152, 153, 154, 155, 156, 157, 158, 159, 160, 161, 162, 163, 164, 165, 166, 167, 168, 169, 170, 171, 172, 173, 174, 175, 176, 177, 178, 179, 180, 181 Clinically, primary iris stromal cysts appear as dome-shaped translucent masses arising from the mid or peripheral surface of the iris. They may appear lobulated and usually contain a clear or slightly turbid fluid, although occasionally they may contain a sediment of white or yellowish material resembling a hypopyon within the cyst155, 171 (Figure 1c). The majority of cases are diagnosed within the first year of life, with occasional cases reported in adults.155 This condition appears to be unilateral in that the author is unaware of any reports of bilateral involvement. In most cases a stromal cyst arises in the inferior or temporal aspect of the iris.155 In general, primary iris stromal cysts, particularly in children, undergo progressive enlargement, which may lead to visual loss when they encroach upon the visual axis.155 Rarely, spontaneous collapse or regression of a stromal cyst has been reported.156, 176, 177 Focal corneal oedema may arise as a result of contact between the stromal cyst and the corneal endothelium.137, 142, 161, 163 Raised intraocular pressure,159, 163, 172, 173 hyphaema137 iritis, and subluxation of the lens163, 167, 171, 173, 174, 175 have been found in association with primary iris stromal cysts.

Although primary iris stromal cysts may develop in adults, they are generally considered to be congenital in origin. Stromal cysts, which arise later in life, have probably been dormant and become apparent as the result of an accumulation of fluid within the cyst, triggered by an unknown stimulus.170 The precise aetiology of primary iris stromal cysts remains unclear and proposed mechanisms include developmental entrapment of surface ectoderm, neuroectoderm, or surface ectodermal implantation as a result of occult trauma.163 Histologically, primary iris stromal cysts are lined with a multi-layered squamous or cuboidal epithelium, which may or may not contain mucin-secreting goblet cells.138, 139, 142, 163, 168, 169, 170, 173, 174, 178, 179 Occasionally, focal keratinisation of the epithelial lining has been observed.170, 180 Immunohistochemical studies have demonstrated a positive reaction for epithelial cytokeratin markers and a negative result for the S100 antigen.159, 163, 166, 170 Electron microscopic studies have shown the presence of microvilli on the luminal surface of the epithelial cells together with desmosomes and tonofilaments.163, 166, 170, 178 These studies support the notion that primary iris stromal cysts originate from the surface ectoderm, displaced probably at the time of formation of the lens vesicle.170 Rummelt et al182 reported two cases of congenital epithelial iris cysts in children who had a maternal history of diagnostic amniocentesis. In one case a perforating limbal scar with a corresponding break in a Descemet's membrane was observed. Lois et al155 in a series of 17 patients with primary iris stromal cysts noted a history of diagnostic amniocentesis in two patients. However, in neither case was there any sign of a penetrating injury to the eye. It would appear that while diagnostic amniocentesis is a possible cause of congenital stromal iris cysts, the majority of cases occur in the absence of any obvious intrauterine trauma.

A wide range of modalities have been used to treat symptomatic primary iris stromal cysts, including simple aspiration,155, 171 and injection with trichloroacetic acid,158 xenon photocoagulation,158 neodymium-YAG laser,164, 171 argon laser photocoagulation,155, 181 cryotherapy,155, 181 iridectomy,158, 142 and block excision.160, 180 Unfortunately, re-occurrence following treatment, particularly simple puncture either surgical or laser, is common and prognosis for vision, particularly in young children where amblyopia may be a problem, is often poor. Recently, Shen et al144 reported a promising surgical technique by using a viscoelastic material to dissect the cyst from the corneal endothelium, followed by aspiration of the cyst, excision, and micro-diathermy.

Posterior cysts

Primary cysts of the IPE or ciliary body have been recognised for over a century.183 In 1897 Zimmerman183 reported a case of bilateral pigmented tumours, which he considered to be ciliary body cysts. Following this report, a number of case reports appeared in the literature noting the appearance of cysts of either the ciliary body or IPE.184, 185, 186, 187 Although initially considered as separate entities, it would now appear that the majority of cysts of the IPE and ciliary body arise from the irido-ciliary sulcus or pars plicata, and should best be considered as irido-ciliary cysts (vide infra). Historically, irido-ciliary cysts were considered to be rare; however, with the advent of the ultrasound biomicroscope it is now recognised that small asymptomatic cysts are extremely common and that only a small proportion of them attain sufficient size or number to become clinically apparent. Recently, Kunimatsu et al188 in a prospective study of 232 eyes of 116 normal subjects by using an ultrasound biomicroscope found evidence of irido-ciliary cysts in 54.3% of patients.

In 1981 Shields140 reported a study of 62 patients with primary iris cysts, of which 59 were considered to have arisen from the posterior pigment epithelium. He classified the pigment epithelial cysts into five groups: central, mid-zonal, peripheral, dislodged into the anterior chamber, and dislodged into the posterior chamber. In a subsequent study using the same classification, Lois et al189 reported the clinical features and the natural course of primary cysts of the IPE in 234 patients. They found central (confined to the pupillary margin) in three patients (6%), mid-zonal cysts in 50 patients (21%), peripheral in 170 patients (73%), and dislodged in eight patients (3%). However, less than 10% of these patients underwent an ultrasound biomicroscope examination to confirm the extent and the posterior origin of the cysts. Subsequent studies using ultrasound biomicroscope would suggest that both peripheral and mid-zonal cysts originate from the irido-ciliary sulcus.190, 191 Indeed, in the author's personal experience, all large cysts involving the mid-zone appear to arise from the irido-ciliary sulcus. It is probable that the majority, if not all, of pigment epithelial cysts (with the exception of those that have become detached and now float in either the vitreous or aqueous) arise either from the pupil margin or the irido-ciliary sulcus. Moreover, as we shall see, the aetiology of these two groups appears to be quite distinct.

Although the majority of small peripheral pigment epithelial (irido-ciliary) cysts are asymptomatic, large cysts can cause focal abnormalities of the iris, which may, on occasion, stimulate an ocular neoplasm. Sadly, prior to the advent of the ultrasound biomicroscope, pigment epithelial cysts had been mistaken for ciliary body melanomas resulting in unnecessary enucleation.186 Clinically, isolated peripheral irido-ciliary cysts present as a focal anterior bulging of the peripheral iris, with an associated shallowing of the anterior chamber. Larger cysts may be visible at the pupil margin, particularly following pharmacological mydriasis. In these circumstances the cyst appears as a smooth uniformly pigmented mass lying between the posterior surface of the iris and the lens. On careful inspection the cyst will usually transilluminate when a fine slit-lamp beam is shone upon its surface. The majority of solitary pigment epithelial cysts appear to arise in the inferior temporal quadrant.189 Bilateral pigment epithelial cysts are common and indeed, when an individual presents with an apparently unilateral lesion, careful inspection of the fellow eye will frequently reveal the presence of an occult lesion in that eye. Occasionally, patients may present with multiple bilateral irido-ciliary cysts191 (Figure 1d) and in extreme cases this may produce a plateau iris leading to angle closure glaucoma.189, 191, 192, 193, 194, 195, 196, 197, 198, 199 Although irido-ciliary cysts are generally sporadic in nature, Vela et al197 reported three families with pigment epithelial cysts, which were multiple in 10 and bilateral in eight of the 11 affected patients. Acute closed angle glaucoma occurred in four of the affected patients.

Although the aetiology of irido-ciliary cysts remains uncertain, numerous theories have been proposed, including; persistence of the annular sinus of von Szily;198 foetal iritis causing synechiae with resultant separation of the two layers of the secondary optic vesicle;200 and embryonic traction of the zonule of Zinn on the posterior epithelial layer of the secondary optic cup.186 It is tempting to speculate that, given peripheral pigment epithelial cysts appear to arise from the irido-ciliary sulcus where there is transition between the non-pigmented epithelium of the ciliary body and the pigment epithelium of the iris, their formation may be due to a focal juxtaposition of these elements, leading to the aberrant secretion of aqueous beneath the pigment epithelium.

While the majority of peripheral pigment epithelial cysts occur in isolation, it is well-recognised that on occasion they may be associated with a ciliary body tumour. Augsburger et al201 noted, in a study by using the ultrasound biomicroscope, that in 39 patients with pigment epithelial cysts, six occurred at the margin of a ciliary body tumour. Fine and Pavlin190 in a further ultrasound biomicroscopic study of 210 irido-ciliary cysts found that 20% were associated with a tumour. While the majority of these cysts are clinically undetectable and can only be diagnosed with the aid of an ultrasound biomicroscope, occasionally iris cysts may be the presenting sign of a ciliary body tumour202 and for this reason it is important to exclude an associated neoplasm in any patient who presents with an apparently isolated pigment epithelial cyst. Moreover, cystic ciliary body melanomas may simulate a pigment epithelial cyst and again this phenomena reinforces the need to undertake a meticulous ultrasound biomicroscope examination in any patient presenting with a solitary cyst.203

Central pigment epithelial cysts, arising from the pupillary margin, are a well-recognised product of miotic therapy. In 1923 Vogt204 described single or multiple cysts at the pupillary margin in patients receiving miotic (pilocarpine) therapy for chronic simple glaucoma. Abraham205 in a study of 66 cases of accommodative strabismus treated with di-isopropyl-fluoro-phosphate noted that pupillary cysts developed in 42 (64%) patients and that occasionally they occur as early as 2 weeks after starting treatment. Chin et al206 reported the occurrence of pupillary cysts in patients receiving phospholine iodide for accommodative strabismus; they noted that this effect could be inhibited by concomitant therapy with the mydriatric phenylephrine. Histologically, the cysts are found to contain finger-like projections consisting of a double layer of pigment epithelial cells enclosing cystic spaces.207

In 1936 Cowan208 described a case of familial cysts and flocculi of the iris. Flocculi have been described as tuft-like excrescences of the pigment epithelium overlying the pupil margin and are often cystic in nature. It is probable that they are aetiologically closely related to simple pigment epithelial cysts and indeed in some articles the term appears interchangeable. More recently, Sallo and Hatvani209 reported four cases of primary pupillary pigment epithelial cysts in a single family. Although there was no mention of any systemic abnormality in this pedigree, several articles have suggested an association between iris flocculi/pupillary pigment cysts and inherited ascending thoracic aortic aneurysms and dissections (TAAD).210, 211, 212, 213, 214 In the past few years several research groups have identified that TAAD may be caused by mutations of the smooth muscle α-actin (ACTA2)213, 214 gene and moreover, that iris flocculi may be specific to the p.R149C mutation.

Vascular tumours and malformations of the iris

Vascular tumours and malformations of the iris are extremely rare. Ashton215 in a pathological study of 145 primary iris tumours found only three primary angiomas of the iris. Indeed, Ferry216 in an archival study concluded that the majority of tumours classified as haemangiomas were in fact juvenile xanthogranulomas, highly vascular melanomas or other non-vascular tumours. However, true vascular tumours and malformations of the iris have been reported in the literature and include capillary,217, 218, 219, 220 cavernous,221, 222, 223, 224, 225, 226 racemose,227, 228, 229, 230, 231 microhaemangiomas,232, 233, 234, 235, 236, 237, 238, 239 and iris varix.240, 241, 242, 243

Capillary haemangiomas are paediatric malformations and appear to arise in association with either diffuse neonatal haemangiomatosis or peri-orbital capillary haemangiomas.217, 218, 219, 220 In general, cavernous haemangiomas arise in adulthood and are not associated with systemic haemangiomas.222, 241 However, sporadic case reports have detailed their association with haemangiomas in other non-ocular sites.241

Microhaemangiomas (iris vascular tufts) are probably the most common vascular malformation to arise in the iris, with a total of approximately 90 reported cases in the literature.234 They typically occur bilaterally and appear as solitary or multiple small (approximately 150 μm in diameter) vascular tufts on the pupil margin. Most cases occur in patients over 50 years of age and indeed, iris microhaemangiomas have not been reported in childhood.234 Although microhaemangiomas have been reported in association with a wide variety of systemic conditions, these are probably, in the majority of cases, merely coincidental, with the possible exceptions of myotonic dystrophy244, 245, 246 and diabetes mellitus.232, 246 Spontaneous hyphaema, which may be complicated by secondary raised intraocular pressure, is a well-recognised complication of iris vascular tufts.237, 239, 247, 248, 249, 250, 251, 252, 253, 254, 255, 256 Iris microhaemangiomas are thought to be hamartomas arising from the stromal blood vessels.235

In 1983 Stur and Strasser227 described a sectorial racemose arterio-venous malformation in a 32-year-old male. Since this report approximately 36 further cases of isolated iris arterial-venous malformation have been reported in the literature.230, 241 These lesions consist of one or more abnormally large iris blood vessels that originate in the iridocorneal angle, which pass through the stroma (which in places may obscure them) towards the pupil margin for a variable distance before forming an abrupt loop and returning to the angle.229 Fluorescein angiography readily identifies these vascular malformations, which fill rapidly and demonstrate no or only minimal leakage or staining of the vessel wall.229 A dilated episcleral vessel in the same quadrant as the arterio-venous malformation was noted in 50% of cases.229 The presence of such a vessel may be confused with sentinel vessels, which are associated with an underlying ciliary body tumour. Iris arterio-venous malformations are not associated with any systemic condition, nor do they give rise to any symptoms.

Iris tumours

Adenomas and adenocarcinomas of the IPE

Adenomas and adenocarcinomas of the IPE are rare. Spraul et al,257 in 1996, reported an adenocarcinoma of the IPE and cited 20 previously reported cases, which would appear to fulfil the criteria to be classified as adenomas of the IPE. Shields et al258 in 1999 reported their personal experience of 20 cases of adenomas arising from the IPE. Since then, only a further single report of an adenoma of the IPE has appeared in the literature.259 The majority of adenomas of the IPE appear to arise from the peripheral iris and may involve the ciliary body. Moreover, adenomas may arise from the pigment epithelium of the ciliary body and, as a result, it is often difficult on clinical grounds to determine which pigment epithelium the tumour has arisen from. Clinically, adenomas of the IPE present as a small asymptomatic mass in the peripheral iris. There appears to be no sex or racial predilection, and typically such lesions present in the fourth to sixth decade of life. Rarely, adenomas may present in childhood and adolescence. We have reported a case of an adenoma, which was composed of pigmented and non-pigmented elements, involving both the iris and the ciliary body, which was probably congenital in origin.260 In most cases adenomas appear as a sharply defined black or dark grey lesion, which has displaced the iris root. The exposed surface of the lesion may be smooth or nodular, and, unlike ciliary body melanomas, there are no associated sentinel vessels. Despite their relatively small size, adenomas of the iris (and ciliary) epithelium frequently erode the iris root giving the appearance of anterior segment invasion. In general, invasion of the iris is a feature of large ciliary body melanomas and thus the finding of a small ‘ciliary body’ tumour in the presence of apparent invasion of the iris root should alert the clinician to the possibility that the lesion is a benign adenoma.261 Adenomas of the IPE appear as homogenous or, occasionally, cystic lesions with a smooth or nodular surface arising from the posterior aspect of the iris. Histologically, adenomas of the IPE appear as deeply pigmented tumours composed of cords and tubules of well-differentiated pigment epithelial cells separated by connective tissue septae. Occasional cystic spaces may be visible within the tumour.258 To the author's knowledge there have been only two reported cases of adenocarcinomas arising from the IPE.257, 262 However, although the histological features were suggestive of a malignant neoplasm, there have been no reported cases of metastases from these tumours, in keeping with adenocarcinomas of the ciliary and retinal pigment.257 Adenomas of the IPE may be treated by surgical resection or observation.258

Iris metastasis

In contrast with the choroid, which is a relatively common site for metastases,263, 264 the iris is rarely involved in the metastatic process. Bloch and Gartner,264 in study of 230 eyes obtained post mortem from patients with confirmed systemic malignancy, found 28 cases of ocular metastases, of which only two (7%) involved the iris. The majority of published cases are confined to single case reports. To date, the largest study in the literature was published by Shields et al,265 who in a study of 512 patients with uveal metastases, found iris involvement in 40 (7.8%) of cases. The breast (40%) and lung (28%) were the most common location for the primary tumour. In approximately one-third of cases, the iris metastasis was the presenting symptom of the underlying malignancy (Figure 1e). In this series 35% of cases had an accompanying choroidal metastasis. The iris metastases were unilateral in all cases. Again, this contrasts with the choroid where bilateral involvement occurs in approximately 30% of cases. Indeed, bilateral iris involvement appears to be extremely uncommon.266, 267, 268

Iris metastases typically appear as a solitary yellow-white or pink fleshy mass on the iris stromal surface. The tumours often appear friable and may liberate cells into the anterior chamber, which can simulate anterior uveitis.265, 269 In addition, iris metastases are capable of invoking a significant inflammatory reaction and as a result may present with a true anterior uveitis.269, 270, 271, 272, 273 Secondary glaucoma is frequently associated with iris metastases occurring in approximately 40% of cases.265 The diagnosis of an iris metastasis may be relatively straightforward when a patient presents with known carcinomatosis, particularly when there is an associated choroidal deposit. However, when the patient presents with a solitary iris lesion in the absence of a history of malignant disease, the diagnosis may be more problematic. In these circumstances a fine-needle aspiration, or punch biopsy, may be of value.265, 274, 275, 276, 277

Melanocytic tumours of the iris stroma


Although iris naevi are undoubtedly common, precise estimates of their prevalence within the general population are lacking. In part, this is due to the fact that the majority of patients with iris naevi are asymptomatic and, as a result, do not seek medical attention. Furthermore, as we shall see, the clinical, and indeed the pathological, distinction between naevi, melanocytomas, and melanomas is somewhat blurred and as a result the precise categorisation of an individual melanocytic iris lesion may be problematic. In a small study, Harbour et al47 found the incidence of iris naevi to be between 4 and 6%. Iris naevi appear to be more common in patients with light-coloured irides47 and individuals with the dysplastic naevus syndrome.278, 279

Clinically, iris naevi may be circumscribed or diffuse in nature and in both forms the lesion effaces or obscures the underlying iris stromal architecture: a feature, which differentiates them from a simple iris ephelis where the architecture is preserved. Circumscribed naevi appear as a well-demarcated lesion, which may vary in size, shape, and degree of pigmentation. The majority of naevi are tan or dark brown in colour, occur in the lower half of the iris, and may involve the pupil margin, mid-zone, or periphery. Traditionally, it has been told that pupillary changes, including corectopia, ectropion uvea, and sector lens opacities, were suggestive of malignancy. However, it is now recognised that such changes may occur in naevi and cannot be used to distinguish benign from malignant lesions.280, 281 Similarly, involvement of the iridocorneal angle, which was again once thought to be indicative of malignancy, may occur in benign naevi.281

Diffuse naevi appear as flat or minimally elevated pigmented lesions, which involve a sector, or occasionally, the entire iris, and are congenital in nature. They are usually encountered in cases of ocular or oculodermal melanocytosis.133 A diffuse iris naevus may also be encountered in Cogan–Reese syndrome. This condition first described in 1969,282 is a variant of the iridocorneal endothelial syndrome, and is characterised by unilateral glaucoma; abnormalities of the corneal endothelium; and iris changes, including, corectopia, ectropion uvea, pigmented nodules, and iris atrophy.283

Iris naevi are generally indolent lesions, which remain asymptomatic throughout life. Occasionally, secondary glaucoma may arise as a result of pigment deposition in the trabecular meshwork. Although rapid tumour growth is considered to be indicative of malignancy, iris naevi may slowly increase in size with time. In a study of 175 melanocytic tumours of the iris, Territo et al284 noted definite tumour growth in eight patients, of which five were treated by iridocyclectomy. Two of these lesions were subsequently found to be spindle cell naevi.

Two reports have now appeared in the literature describing an aggressive naevus of the iris in children. Paridaens et al285 described an apparently unique familial occurrence of an aggressive iris naevus arising in the second decade of life in a mother and son. Carlson et al286 subsequently reported an aggressive iris naevus in a 16-year-old girl who presented with visual loss as a result of uncontrolled secondary glaucoma.

While it is probable that iris naevi may occasionally undergo malignant transformation, it is not possible to estimate how frequently this change occurs. Many iris melanocytic lesions, which histologically appear to be malignant, may remain indolent for many years and as result, should a lesion show a significant increase in size, it may be impossible to determine whether this is due to malignant transformation in a pre-existing naevus of growth in a previously dormant melanoma.


A melanocytoma is a specific type of naevus, which demonstrates characteristic histological features. They are composed of deeply pigmented plump or polyhedral naevus cells, which contain abundant cytoplasm and demonstrate little nuclear pleomorphism.287 Although melanocytomas typically arise on or adjacent to the optic disc, they may occasionally occur in other locations in the eye, including the choroid,288, 289, 290, 291, 292, 293, 294, 295, 296, 297, 298 the ciliary body,299, 300, 301, 302, 303, 304, 305, 306, 307, 308, 309, 310, 311, 312 and the iris.299, 301, 313, 314, 315, 316, 317, 318, 319, 320, 321, 322, 323, 324, 325, 326, 327

In 1965 Zimmerman313 reported an iris melanocytoma in a 34-year-old, which was treated by iridectomy and subsequent enucleation, the initial specimen having been reported to be a malignant melanoma. Since then a number of reports have appeared in the literature documenting the occurrence of melanocytomas within the iris.297, 299, 311, 312, 313, 314, 315, 316, 317, 318, 319, 320, 321, 322, 323, 324, 325 These lesions are, however, uncommon, and in a study of 200 patients referred to an ocular oncology service with the suspected diagnosis of an iris melanoma, 158 were found to have an alternative diagnosis and of these only one proved to be a melanocytoma.328 In a subsequent study of 47 cases of iris melanocytoma, Demirci et al322 estimated that melanocytomas represented only 3% of all iris naevi.

Clinically, iris melanocytomas appear as a darkly pigmented nodule with an irregular or corrugated surface322 (Figure 1f). In keeping with other melanocytic iris lesions, melanocytomas usually involve the inferior half of the iris. These lesions appear to be less cohesive than ordinary naevi and may produce satellite lesions on the iris surface or trabecular meshwork.287 This lack of cohesion may be due to necrosis within the melanocytoma.314, 318, 322, 324 Involvement of the trabecular meshwork may give rise to a raised intraocular pressure.314, 315, 318, 324 Indeed, Demirci et al322 in their study noted that 11% of patients had developed a raised intraocular pressure at 5 and 10 years, and that this had risen to 55% at 15 years. Approximately 50% of iris melanocytomas may demonstrate a gradual enlargement with time,322 and although this is not indicative of malignant transformation, there are sporadic reports of melanomas arising from iris melanocytomas in the literature.316, 325, 329


Iris melanomas are uncommon and account for only between 2 to 5% of all uveal melanomas.330, 331 Despite their relative rarity, iris melanomas remain an enigma and controversy surrounds both their diagnosis and management. Most studies indicate that the mean age of presentation for iris melanomas is 40–45 years: a decade earlier than their posterior uveal counterparts.330, 331, 332 Iris melanomas may be either circumscribed or diffuse, and in both forms the clinical distinction between a melanoma and benign naevus may be difficult.

Circumscribed melanomas have an affinity for the inferior iris and approximately 80% of cases arise from the inferior half of the iris.332 They appear as a raised lesion with either a smooth or irregular surface. The degree of pigmentation is variable and while the majority of iris melanomas are brown in colour, some are amelanotic: the latter often showing a prominent intrinsic vasculature. Pupil distortion, ectropion uveae, localised cataract, iridocorneal angle involvement, pigment dispersion, raised intraocular pressure, and spontaneous hyphaema may be found in iris melanomas.284, 330

Diffuse iris melanomas are extremely rare, accounting for 7–10% of all iris melanomas.330, 333 Clinically, diffuse iris melanomas classically present as a patient with unilateral hyperchromatic heterochromia and ipsilateral glaucoma.333, 334, 335 In affected cases the iris has a diffuse or multifocal pigmentation. Associated corectopia and ectropion iridis occur in approximately 90% of cases and involvement of the iridocorneal angle appears to be a universal feature.333 Unfortunately, there is frequently a significant delay in diagnosing diffuse iris melanomas. Demirci et al333 in a report of 25 cases of diffuse iris melanoma found that 14 (56%) of the cases referred to their unit for further management had previously been diagnosed elsewhere as suffering from glaucoma and that as a result there was a mean delay of 30 months before eventual diagnosis was made. A subsequent review of the literature confirmed a similar delay in diagnosing diffuse iris melanomas.333 This is in keeping with the authors’ own experience where the condition had initially been misdiagnosed as Cogan–Reese syndrome. Histologically, diffuse iris melanomas, in contrast to circumscribed tumours, frequently contain epithelioid cells, which tend to be poorly cohesive and may account for the diffuse nature of these lesions.333

In 1951 Stallard336 wrote that the prognosis for iris melanomas treated by iridectomy was good. A few years later Rones and Zimmerman332 in a retrospective study of 125 cases of iris lesions, which they considered to be either malignant or have malignant potential obtained from the Armed Forces Institute of Pathology files, found the incidence of metastases for patients with iris melanoma to be 1% at 5 years and 6% at 10 years. They observed that the iris melanomas appeared to have a different natural history than their posterior uveal counterparts. Subsequent studies have confirmed that iris melanomas generally have a very favourable prognosis and that the risk of death from metastasis-related disease is small.337, 338, 339, 340, 341, 342, 343 The one exception to this general rule appears to be diffuse iris melanomas where the overall risk of metastases appears to be significantly greater.333

The apparently favourable prognosis for iris melanomas, together with the difficulty in clinically differentiating many lesions from naevi, has prompted many clinicians to adopt a conservative approach to the treatment of such lesions; proposing treatment should rapid growth or other significant complications occur. Traditionally, circumscribed iris melanomas have been treated by iridectomy or iridocyclectomy.331, 332, 333, 334, 335, 336, 337, 338, 339, 340, 341, 342, 343, 344, 345 Alternative treatment modalities include plaque brachytherapy346, 347 and proton beam irradiation.348, 349, 350 The management of diffuse iris melanomas is problematic and most are probably best treated by enucleation, although irradiation may be tried in cases where the patient is reluctant to suffer loss of their eye.333

The apparently low risk of metastatic disease in cases of iris melanoma contrasts with that of choroidal and ciliary body tumours where the mortality rates are significantly greater. In 1992, Diener-West et al351 published a meta-analysis of the 5-year mortality rates among patients who had an eye enucleated for a choroidal melanoma and found the combined weighted estimates to be 16% for small, 32% for medium, and 53% for large tumours. In a recent study of the very-long-term prognosis of patients with choroidal and ciliary body melanoma, Kujala et al352 found tumour-related mortality to be 31% by 5 years, 45% by 15 years, 49% by 25 years, and 52% by 35 years. This, of course, poses the intriguing question as to why there should be such a disparity in relative survivals between iris and posterior uveal melanoma.

Jakobiec and Silbert280 in a retrospective clinical pathological study of 189 iris and iris and ciliary body lesions originally diagnosed as melanomas proposed a new nine part histological classification for such tumours. They subsequently reassigned 87% of the tumours studied into one of six categories, all of which they considered to be benign.280 In doing so they suggested that most iris ‘melanomas’ were in fact benign naevi. If this were indeed the case, then the apparently favourable prognosis for such tumours in previously reported series could be explained by the inclusion of benign lesions into the study groups, which would have the effect of diluting the true malignant neoplasms. While this may the case, it does not entirely explain this paradox. In 2001 Shields et al331 reported the results of a study of 169 consecutive patients with microscopically confirmed iris melanoma and found a metastatic rate of 3% at 5 years and 5% at 10 years, which is remarkably similar to the results found by Rones and Zimmerman332 over 40 years earlier. However, although this excellent study provides us with the incidence of metastatic disease for patients with histologically proven iris melanoma, it suffers from an inherent flaw when considering the overall prognosis for patients with iris melanomas. In this study they obtained the incidence of metastases in 169 patients with histologically proven iris melanoma from a total cohort of 1054 patients referred to the ocular oncology service with suspicious iris melanocytic tumours. The decision to treat or obtain histological biopsy of the lesion was, of course, based on their clinical criteria for possible malignancy. It is of course conceivable that in the remaining 885 patients with the presumptive diagnosis of an iris naevus managed by observation, there may have been patients where the diagnosis would have been that of a melanoma had the tumour been removed and submitted for histological examination.

It is an established fact that tumour size at the time of diagnosis is an important factor in determining the prognosis for posterior uveal melanomas.351 In general, iris melanomas are significantly smaller than most choroidal or ciliary body melanomas at the time of diagnosis, and this has prompted the argument that the apparent difference in biological behaviour can merely be attributed to tumour size. Davidorf353 noted that the mean volume of iris melanomas at the time of diagnosis was 55 mm3 compared with a mean volume of 300 mm3 for choroidal melanomas and concluded that if the size of the tumour at the time of diagnosis was taken into account the metastatic rates would be comparable. Again, the same problem arises: the major criterion for intervention in the case of melanocytic lesion of the iris is documented growth and it is possible that tumours, which histologically would be considered malignant, are left untreated because of the lack of any observable change in size.

In 1990, Prescher et al354 reported apparently non-random chromosome abnormalities in 14 cases of posterior uveal melanoma. Shortly afterwards, my own group reported similar findings in six cases of uveal melanoma.355 Following these initial reports it has now been established that not only do non-random chromosome abnormalities occur in uveal melanomas, but that certain abnormalities, namely loss of chromosome-3 and additional copies of the long arm of chromosome-8, arise predominantly in ciliary body tumours and are highly sensitive predictors of patient survival.356, 357, 358, 359 Unfortunately, to date, there are only two studies (a total of four cases), which have characterised the cytogenetic changes in iris melanomas.360, 361 However, based on this limited evidence it would appear that, although iris melanomas experience relatively high levels of chromosome alterations, they are different to those that are typically found in posterior uveal tumours. If the results of these preliminary results were confirmed in a larger cohort of patients, it could implicate differences in tumour karyotype as a possible cause for the apparent disparity between the metastatic rates of the iris and posterior uveal melanomas.

There is one further intriguing possibility that could explain the apparently different biological nature of the iris and posterior uveal melanomas: could differences in the anterior chamber micro-environment have a role in modulating the behaviour of iris melanomas? Grossniklaus et al362 used a murine model to investigate a difference in metastatic rate between anterior and posterior ocular melanoma, and found that 33% of the tumours inoculated into the anterior chamber metastasised in comparison with 89% of those inoculated into the choroid and/or vitreous. Recently, we have investigated the possible role of the micro-environment in tumour growth. In an in vitro study of the effect of aqueous and vitreous humours on invasion and proliferation, we found that although neither appeared to influence tumour cell proliferation, vitreous promoted tumour invasion whereas aqueous either had no effect or was inhibitory.363 In a further study we identified six enucleation specimens where there was clear invasion of the tumour through the iris stroma and onto the surface. We noted that the surface melanoma cells were smaller when compared with those deeper within the lesion and that fewer of these cells expressed cyclin-D1, a protein that promotes the cell cycle. Moreover, expression of p27, a factor, which inhibits the cell cycle, had a high level of expression in these cells on the anterior tumour surface than those located within the lesion. We also investigated alterations of chromosome-3 and 8, and found them to be less common among the iris surface melanoma cells than those deeper within the body of the tumour.364 Although these results to date must be considered as preliminary, it is plausible that factors within the aqueous humour may have a role in modulating the growth of iris melanomas. If such factors could be identified then they may provide the basis for developing alternative therapies to treat uveal melanoma.