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Hydrogen Sulfide Prevents ATP-induced Neurotoxicity via Inhibiting The NLRP1/caspase-1/gasdermin D-mediated Pyroptosis Pathway
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作者 REN Yan-Kai LI Ying-Hong +4 位作者 LI Man-Li YANG Kun-Li FAN Zhi-Ru ZHANG Si-Yu LI Dong-Liang 《生物化学与生物物理进展》 北大核心 2025年第3期724-734,共11页
Objective Stroke is a leading cause of death and disability worldwide,with ischemic stroke accounting for 80%-85%of cases.Despite the prevalence,effective treatments remain scarce.The compelling evidence suggest that ... Objective Stroke is a leading cause of death and disability worldwide,with ischemic stroke accounting for 80%-85%of cases.Despite the prevalence,effective treatments remain scarce.The compelling evidence suggest that high concentrations of ATP in the brain post-stroke can trigger irreversible neuronal damage and necrosis,contributing to a range of neurocellular dysfunctions.Pyroptosis,a recently identified form of programmed cell death,is characterized by caspase-1 activation and the action of the Gasdermin D(GSDMD)protein family,leading to cell perforation and inflammatory death.Methods In this study,human neuroblastoma SH-SY5Y cells were used to investigate the mechanisms of ATP-induced neurotoxicity and the protective effects of hydrogen sulfide(H_(2)S)against this toxicity through the antagonization of pyroptosis.We employed CCK-8 and LDH assays to assess cell viability.YO-PRO-1 fluorescent dyes and flow cytometry were conducted for detecting changes in cell membrane permeability.Western blot analysis was used to measure protein levels associated with cellular dysfunction.Results Our results indicate that high concentrations of ATP enhance cytotoxicity and increase cell membrane permeability in SH-SY5Y cells,that are mitigated by the H_(2)S donor NaHS.Furthermore,ATP was found to promote the activation of the NOD-like receptor pyrin domain-containing 1(NLRP-1),caspase-1,and the cleavage of GSDMD,with NaHS significantly attenuating these effects.Conclusion Our research suggests that H2S protects SH-SY5Y cells from ATP-induced neurotoxicity through a mechanism mediated by the NLRP1,caspase-1,and GSDMD pathway. 展开更多
关键词 STROKE ATP H2S NLRP1 CASPASE-1 GSDMD PYROPTOSIS
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SSCI不同学科影响因子相关自被引率对比分析 被引量:1
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作者 盛丽娜 顾欢 +1 位作者 刘雪立 王燕 《情报杂志》 CSSCI 北大核心 2018年第4期158-165,共8页
[目的/意义]分析SSCI不同学科影响因子相关自被引率(self-cited rate correlation with impact factor,SCR-IF)的状况,以利于办刊人了解国际优质社会科学期刊不同学科自引的实际状况。[方法 /过程]以2015年版SSCI收录的57个学科期刊为... [目的/意义]分析SSCI不同学科影响因子相关自被引率(self-cited rate correlation with impact factor,SCR-IF)的状况,以利于办刊人了解国际优质社会科学期刊不同学科自引的实际状况。[方法 /过程]以2015年版SSCI收录的57个学科期刊为研究对象,计算各学科内期刊的自被引率(self-cited rate,SCR),同时计算各刊的SCR-IF、非影响因子相关自被引率(self-cited rate non-correlation with impact factor,SCR-NIF)及二者比值K值,对各学科SCR、SCR-IF、SCR-NIF及K值情况作对比分析,同时计算各学科2012-2016年的SCR-IF,以查看近5年的变化趋势。[结果/结论]不同学科间SCR、SCR-IF和SCR-NIF数值差异较大,但各学科SCR-IF均值>SCR均值>SCRNIF均值;各学科平均SCR-IF较SCR-NIF高0.052,较SCR高0.046;SSCI 57个学科中平均K值>2者共15个学科,占26.32%;96.43%(54/56)的学科2016年的SCR-IF较2012年有所降低,平均降低了0.050。SSCI部分学科人为操控自引以提高影响因子的现象应引起注意;SCR-IF较SCR更能敏感地反映出期刊自引对影响因子的实际作用。 展开更多
关键词 影响因子相关自被引率 非影响因子相关自被引率 SSCI 学科评价
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