Schnitzler’s syndrome – diagnostic experience, approaches to therapy, patient management according to a multicenter Russian cohort

S. Salugina, A. Torgashina, E. Borzova, V. Rameev, V. Gorodetskiy, E. Fedorov, N. Muravyeva
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Abstract

The aim – to present the experience of diagnosis, management, and therapy with IL-1 inhibitors in patients with Schnitzler’s syndrome (SchS) according to a multicenter Russian cohort.Materials and methods. In an observational retrospective study for a 10-year period (2012–2022), 17 patients with SchS who were admitted to the hospital or were observed on an outpatient basis, among them 8 women, 9 men, were included in the study. The diagnosis of all corresponded to the Strasbourg diagnostic criteria.Results. The age of patients ranged from 25 to 81 years (Me 53 [46; 56] years). The age at the time of the onset of the disease ranged from 20 to 72 years (Me 46 [39; 54] years), the duration of the disease before diagnosis ranged from 1 to 35 years (Me 6.5 [3; 6] years), in 3 it exceeded 10 years, in the rest it ranged from 1 to 8 years. Infectious and lymphoproliferative diseases, monogenic AIDS (CAPS, TRAPS, HIDS) were excluded from all patients at the prehospital stage. The guiding diagnosis for all was Still’s disease in adults. Clinical manifestations of the disease included: fatigue, lethargy, fatigue, rash and fever in all, skin elements were urticular in all, accompanied by itching in 6 (37.5%). Bone pain had 12 (70.6%), arthralgia – 16 (94.1%), arthritis – 9 (52.9%), myalgia – 7 (41.2%), weight loss in 4 (23.5%). Lymphadenopathy (6), enlarged liver (6), pericarditis (4), angioedema (6), redness and dryness in the eyes (3), sore throat (2), abdominal pain (1), distal polyneuropathy (2), paraesthesia (1), chondritis of the auricles were less common (1). Monoclonal gammopathy was detected in all with a secretion level of 2.9–15.1 g/l: IgMk (n=10 (64.7%)), less often IgMλ (n=2), IgGk (n=2), IgGλ (n=1), IgAλ (n=1). Ben-Jones protein was not detected in any of them. All patients had an increase in the level of ESR, CRP. 16 patients before inclusion in the study received GC (94.1%) with a temporary effect and its escape with dose reduction or cancellation, DMARD – 7, among them methotrexate (5), hydroxychloroquine (2), cyclophosphamide (1), also NSAIDs and antihistamines in all, biological drugs: anti-B-cell the drug rituximab (1), monoclonal AT to IgE – omalizumab in 2 (1 – without effect, 1 – partial effect). 11 patients were prescribed IL-1: canakinumab – 9 (52.9%) subcutaneously once every 8 weeks, anakinra – 4 (23.5%) subcutaneously daily. The duration of taking anakinra, which was prescribed in the test mode, ranged from 1 week to 2.5 months with a further switch to canakinumab in 3. The duration of taking canakinumab at the time of analysis ranged from 7 months to 8 years. Against the background of treatment with IL-1, 10 out of 11 (90.9%) received a complete response from the clinical manifestations of the disease and a decrease in the level of ESR and CRP within a few days. In 1 patient, a partial response was received to the administration of anakinra, and when switching to canakinumab, the effect of treatment was finally lost. 1 patient received IL-6 for 8 months with incomplete effect and transition to IL-1 with positive dynamics. In 1 patient, due to the persistent absence of relapses, the interval between canakinumab injections was increased to 5 months without signs of reactivation, but subsequently, against the background of stress and relapses of the disease, the intervals were reduced to 4 months. A healthy child was born in the same patient on the background of treatment. The tolerability of therapy was satisfactory in all patients, no SAE was noted.Conclusion. SchS is a rare multifactorial/non–monogenic AID that needs to be differentiated from a number of rheumatic diseases and other AIDS. The onset in adulthood, the presence of recurrent urticarial rashes in combination with fever and other manifestations of a systemic inflammatory response are indications for examination for monoclonal secretion. The use of short- or long-acting IL-1 is a highly effective and safe option in the treatment of such patients.
施尼茨勒综合征--根据俄罗斯多中心队列得出的诊断经验、治疗方法和患者管理方法
目的--根据俄罗斯多中心队列,介绍施尼茨勒综合征(SchS)患者的诊断、管理和IL-1抑制剂治疗经验。在一项为期 10 年(2012-2022 年)的观察性回顾研究中,共纳入了 17 名入院或门诊观察的施尼茨勒综合征患者,其中有 8 名女性和 9 名男性。所有患者的诊断均符合斯特拉斯堡诊断标准。患者的年龄从 25 岁到 81 岁不等(平均 53 [46; 56] 岁)。发病时的年龄从 20 岁到 72 岁不等(我为 46 [39; 54]岁),确诊前的病程从 1 年到 35 年不等(我为 6.5 [3; 6]年),其中 3 人的病程超过 10 年,其余人的病程从 1 年到 8 年不等。所有患者在入院前均排除了感染性疾病、淋巴增生性疾病、单基因艾滋病(CAPS、TRAPS、HIDS)。所有患者的指导诊断均为成人斯蒂尔病。该病的临床表现包括:乏力、嗜睡、疲倦、皮疹和发热,所有患者的皮肤均呈荨麻疹状,其中 6 人(37.5%)伴有瘙痒。骨痛 12 例(70.6%),关节痛 16 例(94.1%),关节炎 9 例(52.9%),肌痛 7 例(41.2%),体重减轻 4 例(23.5%)。淋巴结病(6 例)、肝脏肿大(6 例)、心包炎(4 例)、血管性水肿(6 例)、眼睛发红和干涩(3 例)、喉咙痛(2 例)、腹痛(1 例)、远端多发性神经病(2 例)、麻痹(1 例)、耳廓软骨炎(1 例)较少见。所有患者均检出单克隆抗体阳性,分泌水平为 2.9-15.1 克/升:IgMk(10 例(64.7%)),IgMλ(2 例)、IgGk(2 例)、IgGλ(1 例)、IgAλ(1 例)较少见。所有患者均未检测到本琼斯蛋白。所有患者的血沉和 CRP 水平都有所上升。16 名患者在加入本研究前接受了 GC(94.1%)治疗,但效果暂时,随着剂量减少或取消而消失;DMARD - 7 例,其中甲氨蝶呤(5 例)、羟氯喹(2 例)、环磷酰胺(1 例)、非甾体抗炎药和抗组胺药(全部);生物药:抗 B 细胞药物利妥昔单抗(1 例)、抗 IgE 的单克隆 AT - 奥马珠单抗(2 例)(1 例无效,1 例部分有效)。11名患者的处方为IL-1:卡那库单抗--9人(52.9%)每8周皮下注射1次,阿那金拉--4人(23.5%)每天皮下注射1次。以试验模式处方的 anakinra 的服用时间从 1 周到 2.5 个月不等,其中 3 人转为服用 canakinumab。在使用IL-1治疗的背景下,11名患者中有10名(90.9%)在数天内对疾病的临床表现做出了完全反应,血沉和CRP水平也有所下降。有 1 名患者在使用 anakinra 后获得了部分应答,在改用 canakinumab 后,最终失去了治疗效果。1 名患者接受了 8 个月的 IL-6 治疗,但疗效不佳,后转用 IL-1,并取得了积极的动态疗效。在一名患者中,由于持续没有复发,卡那单抗的注射间隔延长至 5 个月,且没有再激活的迹象,但随后在压力和疾病复发的背景下,注射间隔缩短至 4 个月。在治疗过程中,同一名患者生下了一个健康的孩子。所有患者对治疗的耐受性都很满意,未发现任何 SAE。SchS是一种罕见的多因素/非单源性艾滋病,需要与一些风湿性疾病和其他艾滋病区分开来。成年后发病、反复出现荨麻疹并伴有发热和其他全身炎症反应表现是检查单克隆分泌的指征。使用短效或长效 IL-1 是治疗这类患者的一种高效、安全的选择。
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