基于铁死亡探讨防治溃疡性结肠炎的机制

溃疡性结肠炎(ulcerative colitis,UC)是一种慢性炎症性肠道疾病,其病因和发病机制尚未完全明确.随着社会的发展和压力的增加,UC患者数量持续增加,尤其是在亚洲,且与健康个体相比,UC患者患结直肠癌的风险大大增加.虽然目前其具体发病机制尚不清楚,但研究表明与免疫系统、环境、肠道微生态平衡、遗传等多种因素密切相关.UC患者体内与UC模型会发生铁死亡损伤,且在运用铁死亡抑制剂后可有效缓解症状.铁死亡是一种新形式的调节性细胞死亡,是由铁过度积累和脂质过氧化引起的,其特征是铁沉积、脂质过氧化异常和氨基酸代谢异常.本文就铁死亡的三大特征探讨基于铁死亡防治UC的机制及治疗策略作一综述.

浅析细胞自噬在溃疡性结肠炎发病机制中的作用

溃疡性结肠炎是病变累及结直肠黏膜的一种慢性特发性炎性疾病,病情特点是反复发作,主要临床表现为腹痛、腹泻及黏液脓血便等.目前对溃疡性结肠炎的发病机制尚未完全明了,多数学者普遍认为其发病受遗传易感性、环境因素、免疫系统紊乱、微生物组和肠道微菌群失调等因素的影响.近年来,细胞自噬的概念逐渐受到科学界的关注,越来越多的学者在自噬理论的基础上开始研究溃疡性结肠炎的发病机制.本篇综述将从细胞自噬入手浅析其在溃疡性结肠炎发病机制的作用.

NLRP3炎症小体对炎症性肠病免疫机制影响的研究进展

炎症性肠病的发病与机体自身免疫内环境密切相关,而NLRP3炎症小体参与机体的固有免疫应答和T细胞免疫应答.慢性炎症阶段,典型的NLRP3炎症小体被过度激活,增加IL-1β和IL-18从固有层巨噬细胞和树突状细胞中的释放, IL-1β和IL-18的释放可诱导T细胞向致病性Th1和Th17的表型分化,从而维持炎症反应.急性期IL-1β主要以髓系细胞来源促进肠上皮细胞的愈合和修复,即NLRP3炎症小体对肠上皮细胞具有保护性的功能.而同时, NLRP3炎症小体介导的IL-1β的表达导致Th17/Treg失衡,这也与IBD的发病密切相关.可以说NLRP3作为肠内稳态的分子开关,通过IL-1β使局部免疫细胞向炎症表型转变.

KIFC3 promotes proliferation, migration and invasion of esophageal squamous cell carcinoma cells by activating EMT and β-catenin signaling

BACKGROUND Esophageal squamous cell carcinoma(ESCC)is one of the most common malignancies.A total of 45 kinesin superfamily proteins(KIFs)have been identified in humans,among which several family members have demonstrated varied functions in tumor pathobiology via different mechanisms,including regulation of cell cycle progression and metastasis.KIFC3 has microtubule motor activity and is involved in cancer cell invasion and migration,as well as survival.However,the role of KIFC3 in ESCC is still unknown.AIM To evaluate the role of KIFC3 in ESCC and the underlying mechanisms.METHODS Expression of KIFC3 was evaluated in ESCC tissues and adjacent normal esophageal tissues.The prognostic value of KIFC3 was analyzed using Kaplan-Meier Plotter.Colony formation,EdU assays,cell cycle analysis,Transwell assay,immunofluorescence,and western blotting were performed in ESCC cell lines after transfection with pLVX-Puro-KIFC3-shRNA-and pLVX-Puro-KIFC3-expressing lentiviruses.A xenograft tumor model in nude mice was used to evaluate the role of KIFC3 in tumorigenesis.Inhibitor ofβ-catenin,XAV-939,was used to clarify the mechanism of KIFC3 in ESCC.To analyze the differences between groups,t test and nonparametric tests were used.P<0.05 was considered statistically significant.RESULTS Immunohistochemical staining indicated that KIFC3 was upregulated in ESCC tissues compared with adjacent normal tissues.Kaplan-Meier Plotter revealed that overexpressed KIFC3 was associated with poor prognosis in ESCC patients.Colony formation and EdU assay showed that KIFC3 overexpression promoted cell proliferation,while KIFC3 knockdown inhibited cell proliferation in ESCC cell lines.In addition,cell cycle analysis showed that KIFC3 overexpression promoted cell cycle progression.KIFC3 knockdown suppressed ESCC tumorigenesis in vivo.Transwell assay and western blotting revealed that KIFC3 overexpression promoted cell migration and invasion,as well as epithelial-mesenchymal transition(EMT),while KIFC3 knockdown showed the opposite results.Mechanistically,KIFC3 overexpression promoted β-catenin signaling in KYSE450 cells;however,the role of KIFC3 was abolished by XAV-939,the inhibitor of β-catenin signaling.CONCLUSION KIFC3 was overexpressed in ESCC and was associated with poor prognosis.Furthermore,KIFC3 promoted proliferation,migration and invasion of ESCC via β-catenin signaling and EMT.