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B细胞激活因子抑制剂塔巴鲁单抗治疗对等待移植的高度致敏终末期肾病患者的影响。

Effect of Treatment With Tabalumab, a B Cell-Activating Factor Inhibitor, on Highly Sensitized Patients With End-Stage Renal Disease Awaiting Transplantation.

作者信息

Mujtaba M A, Komocsar W J, Nantz E, Samaniego M D, Henson S L, Hague J A, Lobashevsky A L, Higgins N G, Czader M, Book B K, Anderson M D, Pescovitz M D, Taber T E

机构信息

Division of Nephrology, University of Texas Medical Branch, Galveston, TX.

Bio-Medicines Business Unit, Eli Lilly and Company, Indianapolis, IN.

出版信息

Am J Transplant. 2016 Apr;16(4):1266-75. doi: 10.1111/ajt.13557. Epub 2016 Jan 18.

DOI:10.1111/ajt.13557
PMID:26780484
Abstract

B cell-activation factor (BAFF) is critical for B cell maturation. Inhibition of BAFF represents an appealing target for desensitization of sensitized end-stage renal disease (ESRD) patients. We conducted a Phase 2a, single-arm, open-label exploratory study investigating the effect of tabalumab (BAFF inhibitor) in patients with ESRD and calculated panel reactive antibodies (cPRAs) >50%. The treatment period duration was 24 weeks. Eighteen patients received tabalumab, at doses of 240-mg subcutaneous (SC) at Week 0 followed by 120-mg SC monthly for 5 additional months. Patients were followed for an additional 52 weeks. Immunopharmacologic effects were characterized through analysis of blood for HLA antibodies, BAFF concentrations, immunoglobulins, T and B cell subsets, as well as pre- and posttreatment tonsil and bone marrow biopsies. Significant reductions in cPRAs were observed at Weeks 16 (p = 0.043) and 36 (p = 0.004); however, absolute reductions were small (<5%). Expected pharmacologic changes in B cell subsets and immunoglobulin reductions were observed. Two tabalumab-related serious adverse events occurred (pneumonia, worsening of peripheral neuropathy), while the most common other adverse events were injection-site pain and hypotension. Three patients received matched deceased donor transplants during follow-up. Treatment with a BAFF inhibitor resulted in statistically significant, but not clinically meaningful reduction in the cPRA from baseline (NCT01200290, Clinicaltrials.gov).

摘要

B细胞活化因子(BAFF)对B细胞成熟至关重要。抑制BAFF是使致敏终末期肾病(ESRD)患者脱敏的一个有吸引力的靶点。我们进行了一项2a期单臂开放标签探索性研究,调查他巴鲁单抗(BAFF抑制剂)对ESRD且计算群体反应性抗体(cPRA)>50%的患者的影响。治疗期为24周。18名患者接受他巴鲁单抗治疗,第0周皮下注射(SC)240mg,随后连续5个月每月皮下注射120mg。患者再随访52周。通过分析血液中的HLA抗体、BAFF浓度、免疫球蛋白、T和B细胞亚群以及治疗前后的扁桃体和骨髓活检来表征免疫药理学效应。在第16周(p = 0.043)和第36周(p = 0.004)观察到cPRA显著降低;然而,绝对降低幅度较小(<5%)。观察到B细胞亚群的预期药理学变化和免疫球蛋白降低。发生了两例与他巴鲁单抗相关的严重不良事件(肺炎、周围神经病变恶化),而最常见的其他不良事件是注射部位疼痛和低血压。3名患者在随访期间接受了匹配的已故供体移植。使用BAFF抑制剂治疗导致cPRA较基线有统计学意义但无临床意义的降低(NCT01200290,Clinicaltrials.gov)。

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