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利妥昔单抗治疗IgG4相关性疾病:来自连续10例患者的经验教训。

Rituximab for the treatment of IgG4-related disease: lessons from 10 consecutive patients.

作者信息

Khosroshahi Arezou, Carruthers Mollie N, Deshpande Vikram, Unizony Sebastian, Bloch Donald B, Stone John H

机构信息

From Rheumatology Unit (AK, MNC, SU, DBB, JHS), Division of Rheumatology, Allergy, and Immunology, Department of Medicine; and Department of Pathology (VD); Massachusetts General Hospital and Harvard Medical School, Boston, Massachusetts.

出版信息

Medicine (Baltimore). 2012 Jan;91(1):57-66. doi: 10.1097/MD.0b013e3182431ef6.

Abstract

Patients with IgG4-related disease (IgG4-RD) typically have elevated serum concentrations of IgG4 and share histopathologic features that are similar across affected organ(s). IgG4-RD patients frequently require prolonged treatment with glucocorticoids and are often unable to taper these medications. Traditional disease-modifying antirheumatic drugs (DMARDs) are generally ineffective. We assessed the clinical and serologic responses to B lymphocyte depletion therapy in 10 consecutive patients with steroid- and DMARD-refractory IgG4-RD.Ten patients with IgG4-RD were treated with rituximab (RTX) (2 infusions of 1000 mg, 15 days apart). Clinical improvement was assessed by monitoring the patient's ability to taper prednisone to discontinuation and to stop DMARDs; by serial measurements of total IgG and IgG subclasses; and by follow-up radiologic assessments guided by the patient's particular pattern of organ involvement. We also developed and retrospectively applied the IgG4-RD Disease Activity Index and Flare Tool.Organ involvement included the pancreas, biliary tree, aorta, salivary glands (submandibular and parotid), lacrimal glands, lymph nodes, thyroid gland, and retroperitoneum. Nine of 10 patients demonstrated striking clinical improvement within 1 month of starting RTX. One patient with advanced thyroid fibrosis associated with Riedel thyroiditis and a history of disease in multiple other organ systems did not have improvement in the thyroid gland, but the disease did not progress to involve new organs. All 10 patients were able to discontinue prednisone and DMARDs following RTX therapy. Significant decreases in IgG concentrations were observed for the IgG4 subclass only. Four patients were re-treated with RTX after 6 months because of either symptom recurrence and increasing IgG4 concentration at the time of peripheral B cell reconstitution (n = 2) or because of physician discretion (n = 2). Repeated courses of RTX maintained their effectiveness and resulted in further decreases in IgG4 concentrations. In patients who had an increased IgG4 concentration at the time of presentation, the level of serum IgG4 appeared to be a reliable measure of disease activity.IgG4-RD is an idiopathic, multiorgan inflammatory disease in which diverse organ manifestations are linked by characteristic histopathologic and immunohistochemical features. Treatment with RTX led to prompt clinical and serologic improvement in refractory IgG4-RD in all patients with active inflammation. Serial treatments with RTX may lead to progressive declines in serum IgG4 concentrations and better disease control. Serum IgG4 concentrations may remain low, and clinical disease activity may remain quiescent even after B cell reconstitution in a significant proportion of patients.

摘要

IgG4相关疾病(IgG4-RD)患者的血清IgG4浓度通常会升高,且受累器官具有相似的组织病理学特征。IgG4-RD患者常常需要长期使用糖皮质激素治疗,且往往无法逐渐减少这些药物的用量。传统的改善病情抗风湿药(DMARDs)通常无效。我们评估了10例连续的对类固醇和DMARDs治疗无效的IgG4-RD患者接受B淋巴细胞清除疗法后的临床和血清学反应。10例IgG4-RD患者接受了利妥昔单抗(RTX)治疗(2次输注,每次1000mg,间隔15天)。通过监测患者逐渐减少泼尼松用量直至停药以及停用DMARDs的能力来评估临床改善情况;通过连续测量总IgG和IgG亚类;以及根据患者特定的器官受累模式进行随访影像学评估。我们还开发并回顾性应用了IgG4-RD疾病活动指数和复发工具。器官受累包括胰腺、胆管树、主动脉、唾液腺(下颌下腺和腮腺)、泪腺、淋巴结、甲状腺和腹膜后。10例患者中有9例在开始RTX治疗后1个月内表现出显著的临床改善。1例患有与里德尔甲状腺炎相关的晚期甲状腺纤维化且有多个其他器官系统疾病史的患者,甲状腺未见改善,但疾病未进展累及新器官。所有10例患者在RTX治疗后均能够停用泼尼松和DMARDs。仅观察到IgG4亚类的IgG浓度显著下降。4例患者在6个月后因症状复发和外周B细胞重建时IgG4浓度升高(n = 2)或根据医生判断(n = 2)而再次接受RTX治疗。重复使用RTX疗程保持了其有效性,并导致IgG4浓度进一步下降。在就诊时IgG4浓度升高的患者中,血清IgG4水平似乎是疾病活动的可靠指标。IgG4-RD是一种特发性多器官炎症性疾病,其中不同的器官表现通过特征性的组织病理学和免疫组化特征相互关联。RTX治疗使所有有活动性炎症的难治性IgG4-RD患者迅速获得临床和血清学改善。连续使用RTX治疗可能导致血清IgG4浓度逐渐下降并更好地控制疾病。即使在相当一部分患者的B细胞重建后,血清IgG4浓度可能仍保持较低,临床疾病活动可能仍处于静止状态。

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