Effects of carrimycin on biomarkers of inflammation and immune function in tumor patients with sepsis: A multicenter double-blind randomized controlled trial

安慰剂 医学 免疫系统 内科学 败血症 CD8型 胃肠病学 炎症 随机对照试验 不利影响 免疫学 病理 替代医学
作者
Chuanchuan Nan,Xiaowu Zhang,Wei Huang,Biao Zhu,Jianghong Zhao,Song Lu,Lewu Xian,Kaizhong Liu,Gang Ma,Wei Yang,Mingguang Huang,Dongmin Zhou,Ming Zhang,Yan Duan,Guixin Wu,Zhengying Jiang,Li Zhang,Xinrong He,Yuhong Chen,Xue-zhong Xing
出处
期刊:Pharmacological Research [Elsevier BV]
卷期号:198: 106991-106991 被引量:2
标识
DOI:10.1016/j.phrs.2023.106991
摘要

Carrimycin is a potential immune-regulating agent for sepsis in patients with tumors. In this study, we investigated its effects on inflammation and immune function in tumor patients with sepsis. In total, 120 participants were randomized to receive either carrimycin treatment (400 mg/day) (n = 62) or placebo (n = 58) for 7 days. The primary outcomes were immune-related indicators. Subsequently, patients were stratified into two subgroups (CD4 < 38.25% and CD8 < 25.195%). Ninety-nine participants were analyzed: 47 and 52 in the carrimycin and placebo groups, respectively. HLA-DR levels were rapidly increased in the carrimycin group; however, the placebo group initially experienced a decline in HLA-DR level at 1 day after administration. In the subgroup with CD4 < 38.25%, the carrimycin group exhibited significantly higher HLA-DR levels than the placebo group (2.270, P = 0.023) 1 day after administration and the degree of increase in HLA-DR in the carrimycin group was higher than that in the placebo group (2.057, P = 0.040). In the CD8 < 25.195% subgroup, the carrimycin group demonstrated significantly higher levels of CD8+ T cells than the placebo group at 3 (2.300,P = 0.027) and 5 (2.106, P = 0.035) days after administration. Carrimycin intervention led to significant reductions in the SOFA, APACHE II, PCT, and CRP levels. No adverse events were observed. In tumor patients with sepsis, particularly in those experiencing immunological suppression, carrimycin effectively regulates immune responses by increasing HLA-DR and CD8+ T cell levels and plays an anti-infective role, reducing disease severity. (Chictr.org.cn, ID Number: ChiCTR2000032339).
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