zonulin拮抗剂Larazotide(AT1001)作为儿童多系统炎症综合征的辅助治疗:病例系列
Zonulin Antagonist, Larazotide (AT1001), As an Adjuvant Treatment for Multisystem Inflammatory Syndrome in Children: A Case Series.
作者信息
Yonker Lael M, Swank Zoe, Gilboa Tal, Senussi Yasmeen, Kenyon Victoria, Papadakis Lena, Boribong Brittany P, Carroll Ryan W, Walt David R, Fasano Alessio
机构信息
Mucosal Immunology and Biology Research Center, Massachusetts General Hospital, Boston, MA.
Department of Pediatrics, Massachusetts General Hospital, Boston, MA.
出版信息
Crit Care Explor. 2022 Feb 18;10(2):e0641. doi: 10.1097/CCE.0000000000000641. eCollection 2022 Feb.
OBJECTIVES
A recent study suggests that Multisystem Inflammatory Syndrome in Children (MIS-C) is triggered by gastrointestinal breach of severe acute respiratory syndrome coronavirus 2 (SARS-CoV-2) viral particles from the gut lumen into systemic circulation. The virus remains in the gut weeks to months after respiratory infection, causing zonulin release from the intestinal epithelial cells. Zonulin loosens tight junctions, permitting trafficking of highly inflammatory viral particles into circulation. Current MIS-C treatments target the subsequent immune hyperactivation, not the causative loss of mucosal barrier integrity. Larazotide, a zonulin inhibitor, prevents breakdown of tight junctions, limiting antigen trafficking.
DESIGN
Children with MIS-C were treated with larazotide as an adjuvant to steroid/intravenous immunoglobulin therapy. Clinical outcomes, SARS-CoV-2 antigenemia, and cytokine profiles are reported. Outcomes were compared with children with MIS-C receiving steroids and/or IVIG therapy alone.
PATIENTS
Four children with MIS-C, ages 3-17 years, were enrolled.
INTERVENTIONS
Patients were treated with open label larazotide 10 mcg/kg (maximum 500 mcg/dose) orally four times daily for 21 days.
MEASUREMENTS AND MAIN RESULTS
All four patients tolerated larazotide without adverse effects and displayed reduction in Spike antigenemia to undetectable levels. When compared with 22 children with MIS-C receiving steroids and/or intravenous immunoglobulin therapy alone, larazotide-treated patients reported significantly improved time to resolution of gastrointestinal symptoms ( = 0.03), and time to clearance of Spike antigenemia ( = 0.04), plus a trend towards shorter length of stay.
CONCLUSIONS
Larazotide appears safe and well-tolerated and may offer potential benefit as an adjuvant to immune-targeted therapies. Expansion of clinical trials is urgently needed to ascertain the clinical impact of larazotide on MIS-C.
目的
最近一项研究表明,儿童多系统炎症综合征(MIS-C)是由严重急性呼吸综合征冠状病毒2(SARS-CoV-2)病毒颗粒从肠腔经胃肠道进入体循环引发的。呼吸道感染数周乃至数月后,病毒仍留存于肠道,致使肠上皮细胞释放闭合蛋白。闭合蛋白会使紧密连接松弛,从而让高炎性病毒颗粒进入血液循环。目前MIS-C的治疗针对的是后续的免疫过度激活,而非黏膜屏障完整性的病因性丧失。闭合蛋白抑制剂larazotide可防止紧密连接的破坏,限制抗原转运。
设计
采用larazotide对患有MIS-C的儿童进行治疗,作为类固醇/静脉注射免疫球蛋白治疗的辅助手段。报告临床结果、SARS-CoV-2抗原血症和细胞因子谱。将结果与仅接受类固醇和/或静脉注射免疫球蛋白治疗的MIS-C儿童进行比较。
患者
招募了4名年龄在3至17岁的患有MIS-C的儿童。
干预措施
患者接受开放标签的larazotide治疗,剂量为10 mcg/kg(最大剂量500 mcg/剂),口服,每日4次,共21天。
测量指标及主要结果
所有4名患者对larazotide耐受良好,无不良反应,刺突蛋白抗原血症降至无法检测的水平。与22名仅接受类固醇和/或静脉注射免疫球蛋白治疗的MIS-C儿童相比,接受larazotide治疗的患者胃肠道症状缓解时间(P = 0.03)和刺突蛋白抗原血症清除时间(P = 0.04)显著改善,住院时间也有缩短趋势。
结论
Larazotide似乎安全且耐受性良好,作为免疫靶向治疗的辅助药物可能具有潜在益处。迫切需要扩大临床试验以确定larazotide对MIS-C的临床影响。
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