强直性脊柱炎患者血清及关节液中S100A8/9水平变化及意义

目的探讨强直性脊柱炎(AS)患者血清及关节液中S100A8/9水平变化的临床意义。方法选择门诊和住院的AS患者55例,以常用AS疾病活动指数(BASDAI)中位数3.1为界分为活动期组19例和非活动期组36例,选择同期健康体检人员20例作为正常对照组。采用ELISA双抗体夹心法测定S100A8/9水平,采用魏氏法测定ESR,采用Array-360特定蛋白分析仪测定C反应蛋白(CRP)。比较各组血清S100A8/9、CRP和ESR水平,同时比较活动期组患者治疗前后血清S100A8/9水平,并分析其与AS活动参数的相关性。结果 55例患者血清S100A8/9水平高于正常对照组,差异有统计学意义(P<0.01)。15例AS患者关节液中S100A8/9水平高于其血清水平,差异有统计学意义(P<0.01)。活动期组患者血清S100A8/9、CRP和ESR水平均高于非活动期组患者,差异均有统计学意义(均P<0.01)。19例活动期组患者治疗3个月后平均BASDAI值和血清S100A8/9水平均较治疗前下降,差异均有统计学意义(均P<0.01)。55例AS患者血清S100A8/9水平与BASDAI呈正相关(r=0.336,P<0.05),而与ESR、CRP均无相关性(r=0.051和0.067,均P>0.05)。结论 AS患者外周血清S100A8/9水平与疾病活动度密切相关,检测AS患者血清S100A8/9水平对评价疾病活动度和疗效判断有一定价值。

Cmtm4 deficiency exacerbates colitis by inducing gut dysbiosis and S100a8/9 expression

The dysfunction of innate immunity components is one of the major drivers for ulcerative colitis(UC),and increasing reports indicate that the gut microbiome serves as an intermediate between genetic mutations and UC development.Here,we find that the IL-17 receptor subunit,CMTM4,is reduced in UC patients and dextran sulfate sodium(DSS)-induced colitis.The deletion of CMTM4(Cmtm4^(-/-))in mice leads to a higher susceptibility to DSS-induced colitis than in wild-type,and the gut microbiome significantly changes in composition.The causal role of the gut microbiome is confirmed with a cohousing experiment.We further identify that S100a8/9 is significantly up-regulated in Cmtm4^(-/-)colitis,with the block of its receptor RAGE that reverses the phenotype associated with the CMTM4 deficiency.CMTM4 deficiency rather suppresses S100a8/9 expression in vitro via the IL17 pathway,further supporting that the elevation of S100a8/9 in vivo is most likely a result of microbial dysbiosis.Taken together,the results suggest that CMTM4 is involved in the maintenance of intestinal homeostasis,suppression of S100a8/9,and prevention of colitis development.Our study further shows CMTM4 as a crucial innate immunity component,confirming its important role in UC development and providing insights into potential targets for the development of future therapies.

S100A8/S100A9在实体恶性肿瘤化疗疗效中的作用

S100A8和S100A9钙结合蛋白参与调节多种细胞功能,在肿瘤细胞和肿瘤微环境中的差异表达与药物治疗效果密切相关。本文就S100A8、S100A9和S100A8/9二聚体与肿瘤化疗疗效的关系及其可能的相关机制进行综述,以期为耐药性实体恶性肿瘤的治疗提供新思路。

重楼皂苷Ⅶ下调S100A8抑制肺癌转移前微环境形成

目的:评估重楼皂苷Ⅶ干预MDSCs介导转移前微环境形成的作用,揭示"正虚伏毒"转移核心病机的生物学基础。方法:在C57BL/6小鼠上建立皮下移植瘤模型,随机分为4组,分别为生理盐水对照组(NS)、重楼皂苷Ⅶ组(PP7)、紫杉醇组(PTX)、重楼皂苷Ⅶ联合紫杉醇组(PP7+PTX),每组8只,每周给药3次,共用药两周。活体成像检测小鼠成瘤情况,流式细胞术检测外周血MDSCs表达,免疫组化检测MDSCs分泌的相关细胞因子和转移前微环境形成情况。结果:与对照组相比,PP7+PTX组与PP7组均可以控制瘤重(P<0.05),且PP7+PTX组在控制瘤体积方面具有显著性差异(P<0.001);小鼠体重方面无显著性差异;外周血中MDSCs的比例无显著性差异;免疫组化显示,与对照组相比,PP7、PTX、PP7+PTX组均可以下调IDO表达(P<0.01),而PP7+PTX组可下调Arg-1的表达(P<0.05);在转移前微环境方面,免疫组化检测显示,与对照组相比,PP7、PTX、PP7+PTX组均可以下调转移前微环境形成指标S100A8(P<0.05),但对S100A9无显著性差异。结论:重楼皂苷Ⅶ可抑制小鼠皮下瘤生长,并下调S100A8抑制转移前微环境形成,揭示重楼皂苷Ⅶ可能具有扶正的作用,但是否通过调控MDSCs发挥作用尚待进一步探索。

动脉粥样硬化相关血清生物化学及分子生物学检测指标的最新研究进展

动脉粥样硬化是一种在人群中发病率较高的疾病,可以累及全身各处动脉引起相应的并发症,严重危害群体健康。传统的动脉粥样硬化的血清学检测指标仅有助于危险因素的检出,特异度较差。随着研究的进展,新发现许多血清学指标与动脉粥样硬化的发生发展相关,有可能为之后的诊断及后续的靶点治疗提供新的思路和方法,该文就新发现的与动脉粥样硬化相关的血清生物化学及分子生物学检测指标包括S100钙结合蛋白A8和A9,小分子RNA,金属基质蛋白酶MMP-9,微粒MPs及白细胞介素33进行综述。