SARS-CoV-2 Infection in Pemphigus Vulgaris Two Weeks after Rituximab Therapy with Total Recovery: A Case Report.

Lili Róbert, Anikó Kovács, Miklós Sárdy, Melinda Fábián
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In another study, high titers of SARS-CoV-2 antibodies and high counts of antibody-secreting cells were associated with severe COVID-19 (5), which may be the consequence of antibody-dependent enhancement (6). Mahmoudi et al. concluded that B-cells may not be necessary for recovery in COVID-19, but they may protect from reinfection (7). Considering these data, rituximab should be postponed during the pandemic (8). In exceptional cases, it may be applied with careful consideration of the risk-benefit ratio (2,4). Patients should be monitored for signs of COVID-19 before and during treatment. A 63-year-old woman with pemphigus vulgaris presented at our department with widespread skin lesions. Comorbidities included hypertension, hypothyroidism, and glaucoma. Diagnosis was established based on histology and direct and indirect immunofluorescent microscopy results. Both desmoglein-1 and desmoglein-3 autoantibodies were detectable by ELISA. The patient was initially treated with low-dose systemic methylprednisolone (8 mg/day), because glaucoma contraindicated a higher dose. Azathioprine was subsequently started (gradually increased from 0.6 to 2.5 mg/kg/day). Continuous mucocutaneous progression 4 weeks later led to the decision to add rituximab therapy. The patient was confirmed as SARS-CoV-2 negative and received 1000 mg 12 weeks after starting glucocorticoid treatment. Two weeks later, she developed fever and became SARS-CoV-2 positive, and therefore the second rituximab treatment had to be cancelled. The patient had fever for six weeks without any other complaints, hospitalization was not required, and immunosuppression was continued with 8 mg methylprednisolone and 2.5 mg/kg azathioprine. Two weeks after recovery, she was diagnosed with pulmonary embolism, but recovered completely. Pulmonary embolism is a relatively common complication of COVID-19 which may be triggered by inactivity, loss of body fluids due to fever, a hypercoagulable state, and direct toxic venous endothelial damage caused by the virus (9). At a follow-up 4 months later, minimal skin lesions and significantly decreased desmoglein-1 and desmoglein-3 titers were observed. Azathioprine and methylprednisolone therapy were continued, and a second dosage of rituximab was given 7 months from the first one without any side-effects. We conclude that rituximab is a highly effective therapy in pemphigus, but the risk-benefit ratio should be carefully considered during the COVID-19 pandemic. We have not observed irreversible or permanent consequences of its administration, but our patient had a potentially lethal complication, pulmonary embolism, which may be associated with a more severe COVID-19 course due to immunosuppression. 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Abstract

The mortality risk factors for Corona Virus Disease-19 (COVID-19) infection (caused by the severe acute respiratory syndrome coronavirus-2 (SARS-CoV-2)) include advanced age, male sex, certain comorbidities, and immunosuppression (1). Pemphigus vulgaris is a rare mucocutaneous autoimmune disease with autoantibodies against desmosomal desmoglein-1 and desmoglein-3, resulting in acantholysis and blister formation. This epithelial barrier defect increases susceptibility to infections, which may lead to relapses (2). Additionally, therapy-associated immunosuppression can lead to severe infections. Corticosteroids are the mainstay therapy. For moderate and severe pemphigus, rituximab is recommended in first-line treatment along with other immunosuppressants, and it may also be added in refractory cases. It is a monoclonal antibody against CD20 with long-lasting B-cell depletion potency. Recovery of B-cell function may last from one to seven years. Consequently, patients receiving rituximab cannot produce enough COVID-19 specific plasma cells, leading to a severe course of COVID-19 (2). Shashidi-Dadras et al. reported five mild COVID-19 cases among 167 patients with pemphigus who had received rituximab one to five years earlier. The authors presumed rituximab use within five years increases COVID-19 susceptibility regardless the number of courses received (3). Among 48 patients with pemphigus treated with rituximab within five years, Uzuncakmak et al. reported one mild case of COVID-19 (in a patient who had received a single course seven months earlier) (4). In another study, high titers of SARS-CoV-2 antibodies and high counts of antibody-secreting cells were associated with severe COVID-19 (5), which may be the consequence of antibody-dependent enhancement (6). Mahmoudi et al. concluded that B-cells may not be necessary for recovery in COVID-19, but they may protect from reinfection (7). Considering these data, rituximab should be postponed during the pandemic (8). In exceptional cases, it may be applied with careful consideration of the risk-benefit ratio (2,4). Patients should be monitored for signs of COVID-19 before and during treatment. A 63-year-old woman with pemphigus vulgaris presented at our department with widespread skin lesions. Comorbidities included hypertension, hypothyroidism, and glaucoma. Diagnosis was established based on histology and direct and indirect immunofluorescent microscopy results. Both desmoglein-1 and desmoglein-3 autoantibodies were detectable by ELISA. The patient was initially treated with low-dose systemic methylprednisolone (8 mg/day), because glaucoma contraindicated a higher dose. Azathioprine was subsequently started (gradually increased from 0.6 to 2.5 mg/kg/day). Continuous mucocutaneous progression 4 weeks later led to the decision to add rituximab therapy. The patient was confirmed as SARS-CoV-2 negative and received 1000 mg 12 weeks after starting glucocorticoid treatment. Two weeks later, she developed fever and became SARS-CoV-2 positive, and therefore the second rituximab treatment had to be cancelled. The patient had fever for six weeks without any other complaints, hospitalization was not required, and immunosuppression was continued with 8 mg methylprednisolone and 2.5 mg/kg azathioprine. Two weeks after recovery, she was diagnosed with pulmonary embolism, but recovered completely. Pulmonary embolism is a relatively common complication of COVID-19 which may be triggered by inactivity, loss of body fluids due to fever, a hypercoagulable state, and direct toxic venous endothelial damage caused by the virus (9). At a follow-up 4 months later, minimal skin lesions and significantly decreased desmoglein-1 and desmoglein-3 titers were observed. Azathioprine and methylprednisolone therapy were continued, and a second dosage of rituximab was given 7 months from the first one without any side-effects. We conclude that rituximab is a highly effective therapy in pemphigus, but the risk-benefit ratio should be carefully considered during the COVID-19 pandemic. We have not observed irreversible or permanent consequences of its administration, but our patient had a potentially lethal complication, pulmonary embolism, which may be associated with a more severe COVID-19 course due to immunosuppression. Total recovery was observed despite COVID-19 shortly after the initiation of rituximab.

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接受利妥昔单抗治疗两周后完全康复的丘疹性荨麻疹中的 SARS-CoV-2 感染:病例报告。
科罗娜病毒病-19(COVID-19)感染(由严重急性呼吸系统综合征冠状病毒-2(SARS-CoV-2)引起)的死亡风险因素包括高龄、男性、某些合并症和免疫抑制(1)。丘疹性荨麻疹是一种罕见的皮肤黏膜自身免疫性疾病,患者体内存在针对去鳞屑蛋白-1(desmosomal desmoglein-1)和去鳞屑蛋白-3(desmoglein-3)的自身抗体,从而导致棘层溶解和水疱形成。这种上皮屏障缺陷增加了感染的易感性,可能导致复发(2)。此外,与治疗相关的免疫抑制也会导致严重感染。皮质类固醇是主要的治疗方法。对于中度和重度丘疹性荨麻疹,建议在一线治疗中使用利妥昔单抗和其他免疫抑制剂,对于难治性病例也可添加利妥昔单抗。利妥昔单抗是一种抗 CD20 的单克隆抗体,具有长效的 B 细胞耗竭作用。B 细胞功能的恢复可持续 1 到 7 年。因此,接受利妥昔单抗治疗的患者无法产生足够的 COVID-19 特异性浆细胞,从而导致严重的 COVID-19 病程(2)。Shashidi-Dadras 等人报告了 167 名接受利妥昔单抗治疗 1 至 5 年的丘疹性荨麻疹患者中的 5 例轻度 COVID-19 病例。作者推测,无论接受了多少个疗程的利妥昔单抗治疗,五年内使用利妥昔单抗都会增加 COVID-19 的易感性(3)。在五年内接受利妥昔单抗治疗的 48 名丘疹性荨麻疹患者中,Uzuncakmak 等人报告了一例轻度 COVID-19 病例(患者在七个月前接受过一个疗程的治疗)(4)。在另一项研究中,高滴度的 SARS-CoV-2 抗体和高数量的抗体分泌细胞与严重的 COVID-19 相关(5),这可能是抗体依赖性增强的结果(6)。Mahmoudi 等人的结论是,B 细胞可能不是 COVID-19 康复所必需的,但它们可以防止再次感染(7)。考虑到这些数据,大流行期间应推迟使用利妥昔单抗(8)。在特殊情况下,可在仔细考虑风险效益比后使用利妥昔单抗(2,4)。在治疗前和治疗期间,应监测患者是否出现 COVID-19 征兆。一名患有寻常性丘疹性荨麻疹的 63 岁女性患者因广泛的皮损到我科就诊。合并症包括高血压、甲状腺功能减退症和青光眼。根据组织学以及直接和间接免疫荧光显微镜检查结果确定了诊断。通过酶联免疫吸附试验(ELISA)可检测到去甲斑鸠蛋白-1 和去甲斑鸠蛋白-3 自身抗体。患者最初接受了小剂量全身甲基强的松龙(8 毫克/天)治疗,因为青光眼禁忌大剂量治疗。随后开始使用硫唑嘌呤(从 0.6 毫克/千克/天逐渐增加到 2.5 毫克/千克/天)。4 周后,患者的粘膜病情持续恶化,因此决定增加利妥昔单抗治疗。患者被确诊为 SARS-CoV-2 阴性,并在开始糖皮质激素治疗 12 周后接受了 1000 毫克的治疗。两周后,她出现发热并转为 SARS-CoV-2 阳性,因此不得不取消第二次利妥昔单抗治疗。患者发热六周,无其他不适,无需住院治疗,继续使用 8 毫克甲基强的松龙和 2.5 毫克/千克硫唑嘌呤进行免疫抑制。康复两周后,她被诊断为肺栓塞,但已完全康复。肺栓塞是 COVID-19 比较常见的并发症,其诱因可能是缺乏活动、发烧导致体液流失、高凝状态以及病毒造成的直接毒性静脉内皮损伤(9)。在 4 个月后的随访中,观察到的皮损极少,去甲斑蝥素-1 和去甲斑蝥素-3 滴度明显下降。患者继续接受硫唑嘌呤和甲基强的松龙治疗,并在第一次用药 7 个月后第二次使用利妥昔单抗,但未出现任何副作用。我们的结论是,利妥昔单抗是治疗丘疹性荨麻疹的高效疗法,但在 COVID-19 大流行期间,应仔细考虑其风险效益比。我们没有观察到使用利妥昔单抗会造成不可逆转或永久性的后果,但我们的患者出现了潜在的致命并发症--肺栓塞,这可能与免疫抑制导致的更严重的 COVID-19 病程有关。在开始使用利妥昔单抗后不久,尽管使用了 COVID-19,患者仍完全康复。
本文章由计算机程序翻译,如有差异,请以英文原文为准。
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