Abstract
Chronic graft-versus-host disease (cGVHD) is one of the major causes of late mortality after allogenic hematopoietic stem cell transplantation. Moderate-to-severe cGVHD is associated with poor health-related quality of life and substantial disease burden. While corticosteroids with or without calcineurin inhibitors comprise the first-line treatment option, the prognosis for patients with steroid-refractory cGVHD (SR-cGVHD) remains poor. The mechanisms underlying steroid resistance are unclear, and there are no standard second-line treatment guidelines for patients with SR-cGVHD. In this review, we provide an overview on current treatment options of cGVHD and use a series of theoretical case studies to elucidate the rationale of choices of second- and third-line treatment options for patients with SR-cGVHD based on individual patient profiles.
Introduction
The use of allogenic hematopoietic stem cell transplant (allo-HSCT) for treatment of malignant and non-malignant conditions continues to increase annually due to significant improvement in early mortality [1], but moderate or severe chronic graft-versus-host disease (cGVHD) remains a major limitation for broadening the allo-HSCT clinical application [2] with patients developing steroid-refractory cGVHD (SR-cGVHD) having a significantly increased morbidity and mortality [3]. SR-cGVHD has been defined as cGVHD progression while on prednisone at ≥1 mg/kg/day for 1–2 weeks, or stable cGVHD while on ≥0.5 mg/kg/day for 1–2 months, and additional patients remain steroid-dependent with repeated symptom flares during taper of corticosteroids below 0.25 mg/kg/day [4].
The National Institutes of Health (NIH) consensus criteria define acute GVHD (aGVHD) and cGVHD based on a combination of clinical features and time of onset [5]. Approximately 30–70% of allo-HSCT recipients surviving at least 100 days post-transplant develop cGVHD [6]. Increasing rates have been reported in recent decades [7] due to several factors, including increased use of granulocyte colony-stimulating factor mobilized blood stem cells as the graft source, increased patient´s age, and use of unrelated as well as HLA-mismatch donors with the previous aGVHD, further increasing risk [8, 9].
Unlike in aGVHD, the underlying pathogenesis of cGVHD is not well understood, but is thought to be complex and multifactorial, with involvement of T and B cells as well as innate responses, including the transition from inflammation to fibrosis involving fibroblasts and macrophages [10,11,12]. Decreased regulatory T cells (CD4 + CD25 + ) have been observed in cGVHD, which may increase the proliferation of type 1 T cells [13]. Increased levels of transforming growth factor-β are observed in patients with cGVHD compared with healthy controls, although its role in disease pathogenesis has not been established [14, 15]. Additionally, auto-antibody production by host-reactive B cells and plasmablasts, fibrotic changes following type 2 donor responses, and thymic damage impairing immune-reconstitution contribute to the pathogenesis [10, 15]. Figure 1 contains a summary of the pathophysiology of cGVHD including treatment options targeting specific pathways.
CNI calcineurin inhibitors, cyclo. cyclophosphamide, ECP extracorporeal photopheresis, IL-2 interleukin-2, IL17 interleukin 17, imids immunomodulatory imide drugs, MMF mycophenolate mofetil, MSC mesenchymal stromal cells, mTOR-Inh. mechanistic target of rapamycin inhibitors, MTX methotrexate, PDGFα platelet-derived growth factor receptor alpha, TGFβ transforming growth factor β, TLR Toll-like receptor, TNFα tumor necrosis factor alpha, TNI total nodal irradiation. mTOR-Inh.: sirolimus, everolimus; imids: thalidomide, pomalidomide; proteosome inhibitors: bortezomib, ixazomib. It should be noted that listing of one target does not exclude additional targets in specific drugs (i.e. proteosome inhibitors target T cells, B cells, and plasma cells).
There is also an emerging understanding of the role of the gut microbiome on cGVHD presentation [16]. Loss of flora diversity following allo-HSCT has been associated with the development of aGVHD and cGVHD, as well as increased mortality risk [17]. However, the specific role of these intestinal changes in cGVHD has not been studied as thoroughly as in aGVHD.
Signs and symptoms of cGVHD can be stratified as diagnostic, distinctive, and those in common with aGVHD [5], but patients can also show manifestations of other immune-mediated disease such as Hashimoto’s thyroiditis or glomerulonephritis (“other/associated” manifestations) [4]. Correct diagnosis is crucial for the treatment of cGVHD. Of note, a significant proportion of patients lack diagnostic signs of cGVHD and several case series showed that a relevant subgroup of patients being treated for cGVHD in the absence of histopathological confirmation had other diseases, not GVHD [18, 19]. Therefore, patients not responding to treatment for suspected cGVHD and lacking diagnostic symptoms, should be re-evaluated by histopathology [20, 21].
Clinical features may affect multiple organs or body areas, with varying presentation depending on the site involved [6, 10]. The skin is most commonly affected, observed in up to 75% of cGVHD cases; symptoms and signs include poikiloderma, lichen planus-like eruptions, sclerotic features, and depigmentation [5]. The presence and severity of organ-specific signs and symptoms (NIH score 0 to 3) contribute to the NIH global severity of cGVHD (mild, moderate, or severe) [5]. While overall severity has a significant impact on morbidity and mortality, additional risk factors for increased mortality consistently reported include direct progression from aGVHD to cGVHD, and platelets <100/nL at time of diagnosis [22]. Moreover, certain organ involvement such as the lung and gastrointestinal tract, and hyperbilirubinemia are associated with a poor prognosis [23].
In addition to organ impairment caused by cGVHD, patients often have comorbidities associated with treatment, such as osteoporosis induced by corticosteroids [7]. Overall, cGVHD is associated with considerable patient burden and impacts health-related quality of life, depending on the clinical features experienced, and reduced health-related quality of life correlates with increased disease severity and lack of response to treatment [24, 25]. Patients frequently report reduced functional capabilities [26], psychological distress [27], and negative mood [26]. Furthermore, cGVHD has been associated with diagnoses of disabilities including keratoconjunctivitis sicca, sclerosis, and reduced lung function [28, 29]. Uninsured patients may also face a substantial financial burden from cGVHD due to high treatment costs [30].
Standard GVHD prophylaxis for HLA-matched transplants comprises a calcineurin inhibitor plus a short course of methotrexate or mycophenolate mofetil (MMF) with or without additional antithymocyte globulin (ATG) in transplants from unrelated donors; ATG has recently been also recommended for use in HLA-identical sibling transplantation [31]. The aim of these prophylactic treatments is to reduce the risk of aGVHD, one of the major risk factors for cGVHD which continue to manifest in approximately half of the patients [32]. Nevertheless, several approaches have resulted in decreased rates of cGVHD, including the use of ATG as part of GVHD prophylaxis [33,34,35,36] and post-transplant cyclophosphamide in combination with a calcineurin inhibitor (with or without MMF), even in the peripheral blood stem cell transplantation setting and naïve T-depleted grafts [37]. Post-transplant cyclophosphamide has also increased the number of haplo-identical donors without any increases in rates of cGVHD [38, 39]. However, a significant percentage of patients will develop moderate-to-severe cGVHD [40, 41]. Early intervention can ameliorate symptoms and improve survival rates for patients who develop cGVHD [5]. Patients with mild cGVHD may only require treatment with local therapies such as topical steroids, depending on the organ or site affected and on the risk of relapse of the underlying disease [42]. The recommended first-line treatment for moderate or severe disease is systemic corticosteroids (prednisone) with or without a calcineurin inhibitor [3, 31, 42]. Overall, only 40–50% of patients respond adequately to first-line treatment, and over half become steroid-resistant or -dependent, requiring second-line treatment within 2 years due to suboptimal responses, loss of response, or unsuccessful steroid tapering [3, 6]. Additionally, the long-term use of immunosuppressants, including steroids, has been associated with significant toxicity and increased risk of infection [10].
The mechanisms of steroid resistance in cGVHD are not well described [43], and prognosis remains poor for individuals with SR-cGVHD. Steroid resistance has been characterized in many inflammatory diseases such as asthma, chronic obstructive pulmonary disease, and rheumatoid arthritis [44]. To date, several underlying mechanisms have been identified for these conditions, including activation of mitogen-activated protein kinase, reduced histone deacetylase-2 expression, activation of transcription factor activator protein 1, and increased P-glycoprotein-mediated drug efflux [44]. It is yet to be investigated whether any of these mechanisms play a role in GVHD. While we are not aware of any studies into the mechanisms of steroid resistance in cGVHD, murine models have been developed for aGVHD [43]. Despite the key role of T cell responses in aGVHD, these models showed no significant association with donor T cell characteristics, inflammatory cytokine levels, or timing of steroid initiation [43], whereas increasing evidence underlines the role of myeloid cells and fibroblasts [45]. While steroid-resistant cGVHD, as defined by a lack of response to steroids, is challenging, a significant number of patients respond to a regimen of increased steroids. However, exacerbations of cGVHD are frequent when steroid withdrawal is attempted, resulting in significant long-term morbidity due to prolonged use of steroids. Research on the mechanisms of steroid-refractoriness and -dependence remains ongoing and will aid in developing treatments to overcome steroid resistance. Another clinical challenge in SR-cGVHD remains the non-reversibility of certain organ manifestations [24, 46], such as severe ocular involvement which rarely responds to immunosuppressive treatment, and deep cutaneous sclerosis showing a protracted response, if any [3]. The same applies for pulmonary manifestations, with stabilization of the condition regarded as a success, which impairs appraisal of the treatment efficacy [47].
There are no standard second-line treatments for patients with SR-cGVHD. While an increasing number of treatment options are becoming available, data are limited, and no consensus has been found on an optimal approach; these circumstances lead to a wide variation in individual clinical practice [3, 31, 48]. Numerous clinical trials have been performed to evaluate interventions [49], and results from retrospective and prospective studies often report high response rates, but are difficult to interpret due to variations in study design and populations treated [50]. Table 1 outlines some of the main second- and third-line treatment options currently available for SR-cGVHD. The choice of treatment for SR-cGVHD is largely patient-specific and based on several factors, including clinical experience and published evidence, risk profile, disease history, comorbidities, individual tolerance to medication, and access to ongoing clinical trials [51]. Currently, ibrutinib, a Bruton’s tyrosine kinase and interleukin-2-inducible T cell kinase inhibitor, is the only FDA-approved therapy for SR-cGVHD. Ibrutinib targets both B and T cells, making it an attractive option for manifestations that involve auto-antibody production.
In the second section of this review, we discuss three case studies of patients with SR-cGVHD from our clinics and suggest potential treatment options based on their individual profiles.
Case presentation
Patient 1
Patient 1 is a 74-year-old male former smoker who received a peripheral blood HLA-mismatched graft from an unrelated female donor. He was initially treated for quiescent onset of moderate cGVHD (skin grade 2, mouth grade 1, and lung grade 1) starting 10 months after transplantation, with 1 mg/kg/day prednisone tapered to 0.25 mg/kg/day plus tacrolimus and fluticasone, azithromycin, and montelukast therapy. He then developed a > 15% decline in forced expiratory volume in 1 second (FEV1) with steroid taper, FEV1 of 44%, FEV1/forced vital capacity of 0.62 (grade 2), moderate mouth symptoms with lichenoid features and ulceration (grade 2), and deep sclerotic features on lower limbs (grade 3). He has an active fungal lung infection and confirmed cytomegalovirus reactivation.
Treatment options
Patients with SR-cGVHD should ideally be enrolled in a clinical trial; however, this case would most likely not meet eligibility criteria due to the active fungal infection. Despite the greater efficacy of ruxolitinib than best available therapy in patients with SR-cGVHD [52], the patient’s active fungal and viral infections cause some reluctance for use of ruxolitinib, ibrutinib, or MMF due to a further increase in risk for exacerbation of the ongoing infections. Given the severity of his baseline airway obstruction, the possibility of further bronchiolitis obliterans syndrome progression despite active fungal infection, and his poorly controlled cGVHD (affecting extrapulmonary sites), we would favor prompt initiation of extracorporeal photopheresis (ECP). ECP has been assessed in both steroid-dependent- and SR-cGVHD patients [53] and has demonstrated efficacy and safety in the treatment of bronchiolitis obliterans syndrome following HSCT and lung transplantation [54, 55]. It has also shown significant response rates in patients with sclerodermatous and mucosal GVHD in previous studies, including a randomized phase 2 trial [53, 56]. ECP increases regulatory T cells, with beneficial effects reported in patients with sclerotic SR-cGVHD [53]. ECP is associated with very low rates of infectious complications and has a steroid-sparing effect in cGVHD, which is particularly appropriate for this case [53, 55]. Among the many different schedules reported for ECP delivery, we usually administer it twice weekly for the first month and then twice weekly every other week for 6 to 12 months. Once ECP is initiated, we also pursue steroid tapering as soon as possible, to reduce the impact on the treatment of his fungal infection and to avoid new cytomegalovirus reactivation episodes. To monitor lung response and guide steroid tapering or further therapy, we would order pulmonary function tests at least every 4 weeks during the first 3 months. We would consider ECP discontinuation only if GVHD progresses after at least 3 months of therapy.
Patient 2
Patient 2 is a 58-year-old male who received a reduced-intensity peripheral HSCT graft from his HLA-identical sister and GVHD prophylaxis with cyclosporine (CSP) and MMF. He developed steroid-sensitive classic grade 2 aGVHD (skin grade 2, gut grade 1) on day + 53 and presented 18 months after transplantation with quiescent onset of high risk cGVHD, including elevated bilirubin > 3 mg/dl (grade 3) plus fasciitis affecting wrists, elbows, and shoulders, with moderate limitation in the photographic range of motion scale (P-ROM) of 16 (grade 2), while still receiving treatment with low-dose corticosteroids and sirolimus. Both episodes (aGVHD and cGVHD), which were initially treated with prednisone 1 mg/kg/day, were complicated by latent steroid-psychosis requiring a rapid taper of steroids and combination treatment. The patient also experienced impaired renal function on CSP. At the time of cGVHD progression, immunoglobulins (Ig) were above the normal range, with concurrent elevated IgG1 and IgG2 deficiency. The patient also had an expanded CD19+ B cell count, normal CD4+ T cell counts, platelets 75/nl, and granulocytes 1.5/nl. Screening for liver-directed autoantibodies confirmed the presence of a significant titer of antinuclear and anti-smooth-muscle antibodies.
Treatment options
In this case, as the patient is thrombocytopenic, FDA-approved ibrutinib is not the most suitable option. While ibrutinib targets both B cells and plasmablasts, it also interferes with platelet function, which may increase the risk of bleeding complications [57]. While MMF could be an option because of evidence from autoimmune hepatitis [58], the potential cytostatic effect of MMF may promote cytopenia already present. Additionally, while ECP could be beneficial for this patient, it requires time to reach a response and may be ineffective when given alone.
Therefore, we decided to treat the patient with a course of rituximab combined with ruxolitinib and to continue low-dose steroids because of prior intolerance. While ruxolitinib has been shown to be an effective immunosuppressive agent targeting T cells and macrophages (both involved in cGVHD, including sclerosis), it also may indirectly target B cells, which are thought to be involved in this patient, by blocking follicular T helper cells inducing new B cells [59]. The combination would permit the initial depletion of a significant proportion of autoreactive B cells followed by a blockage of new “supply”. Moreover, ruxolitinib has been associated with reactivation of prior seroconverted hepatitis B, indicating a suppressive effect on the humoral-mediated immune mechanism [60]. However, this strategy poses significant infectious risks, as both agents have been associated with infectious complications [61]. Therefore, proper infection prophylaxis (Pneumocystis jirovecii pneumonia, varicella-zoster virus) and continuing antibiotic prophylaxis is mandatory, and substitution of Ig in the presence of bacterial infection complications to resolve the IgG2 deficiency is indicated. Ruxolitinib also requires monitoring of blood counts and liver enzymes, as the patient already has cytopenia and impaired liver function, predisposing him to side effects.
Patient 3
Patient 3 is a 66-year-old female who received a matched unrelated donor peripheral blood HSCT. She has active cGVHD with fibrotic and inflammatory manifestations despite 3 months of treatment with prednisone 0.5 mg/kg/day and continued prophylactic CSP. Five months post-transplant, she presented with the following symptoms: morphea-like superficial sclerotic features in the skin plus lichen sclerosus (40% body surface; grade 2); moderate mouth symptoms with lichenoid features (grade 2); vulvar lichen sclerosus-like features and mild discomfort (grade 1); and moderate dry eye symptoms with corneal keratinization but no vision impairment (grade 2). Pre-existing comorbidities include type 2 diabetes, avascular necrosis, and neutropenia.
Treatment options
Due to lack of evidence to guide which therapy is superior for this patient specifically, we would first consider treatment in a clinical trial as an option for this case. We would replace CSP with another treatment, as CSP failed to control the progression and potentially impedes the emergence of regulatory T cells, which are involved in the pathobiology of cGVHD [24]. Another consideration is to add a secondary therapy with a steroid-sparing effect, as this patient has diabetes and is at increased risk for prolonged systemic treatment including corticosteroids, because she received a peripheral blood HSCT instead of bone marrow transplant [62]. Finally, the treatment for this patient should be an agent that targets the pathobiology of sclerotic cGVHD phenotypes and has a reported beneficial effect in this clinical setting.
Several treatment options are available for this case. Ruxolitinib targets several signaling pathways involved in the pathobiology of cGVHD and has demonstrated superior efficacy than the best available therapy in patients with cGVHD in a recent phase 3 clinical trial [52]. Ruxolitinib may therefore be the preferred therapy option for this case, although the patient should be monitored for neutropenia and increased infection risk [52]. Alternatively, ibrutinib targets T and B cell signaling pathways and has reported responses in patients with sclerotic manifestations [63, 64]. We would start ibrutinib at a dose of 280 mg once daily plus anti-mold infection prophylaxis (i.e., voriconazole 200 mg twice daily, or posaconazole 100 mg twice daily), because of the concern of early invasive fungal infections [65]. Other treatment options include ECP or other treatments that increase regulatory T cells, such as interleukin-2, which has also shown benefit in patients with sclerotic SR-cGVHD [66]. Rituximab, which has demonstrated initial high responses in retrospective studies (but lower responses in prospective studies) for sclerotic SR-cGVHD [67, 68] could also be considered if the treatments previously discussed are not suitable. Finally, MMF in combination with steroids could also be an option if other options are not feasible, but its efficacy for sclerotic cGVHD has not been tested prospectively.
A final important point for management of this case is to optimize supportive care [69], such as through the use of topical dexamethasone oral rinses together with oral nystatin to prevent/treat superimposed yeast infection for oral manifestations, application of topical betamethasone for the vulva [69], and supportive ocular treatment including the use of eye lubricant, CSP ophthalmic emulsion, ocular punctal plugs, scleral lens, and other care [70].
Conclusion
In summary, these three patient cases illustrate multiple options available for patients with SR-cGVHD. While there is one FDA-approved treatment currently available, enrollment in ongoing clinical trials is also an important option for eligible patients whose treatment has failed on one or more previous therapies. In the absence of robust evidence of benefits for any one intervention, treatment choices should be based on physician experience, ease of use, need for monitoring, risk of toxicity, and potential worsening of pre-existing comorbidities.
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Acknowledgements
This work was supported by Novartis AG. The authors would like to thank Keisha Peters, MSc, and James Matthews, PhD, of Excerpta Medica, for editorial assistance in the preparation of this manuscript, supported by Novartis AG.
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D.W. has received honoraria from MACO, Mallinckrodt, Neovii Pharmaceuticals, Novartis AG, and Takeda Pharmaceutical Company Limited. G.F. has an advisory role and has served on speakers’ bureaus for Janssen Global Services LLC. N.K. has received research support from Celgene, Novartis AG and RIEMSER Pharma GmbH; speaker honoraria from Bristol-Myers Squibb Company, Celgene Corporation, Gilead Sciences Inc., Janssen Global Services LLC, Kite, Neovii Pharmaceuticals, Novartis AG, and Sanofi. MEF has received research support from Incyte and Pharmacyclics LLC including AbbVie Inc.; speaker honoraria from Astellas Pharma US, Inc., Janssen Global Services LLC, and Mallinckrodt; and served as a consultant for CSL Behring, Fresenius Kabi AG, and Pharmacyclics LLC. V.R. has no conflict of interest to report.
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Wolff, D., Fatobene, G., Rocha, V. et al. Steroid-refractory chronic graft-versus-host disease: treatment options and patient management. Bone Marrow Transplant 56, 2079–2087 (2021). https://doi.org/10.1038/s41409-021-01389-5
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DOI: https://doi.org/10.1038/s41409-021-01389-5
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