幽门螺杆菌感染策略及宿主细胞对CagA癌蛋白反应的研究

Hitoshi Tsugawa
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引用次数: 2

摘要

慢性幽门螺杆菌感染涉及多种临床结果,包括胃癌。在本研究中,我们主要关注幽门螺杆菌感染策略与慢性感染的建立。结果,揭示了以下四个发现。1) α -酮戊二酸氧化还原酶(KOR)是幽门螺杆菌球虫形式能量代谢的必需生存酶,KOR活性的失活可通过阻止球虫形式的诱导对幽门螺杆菌产生有效的杀菌作用。2)铁摄取调节剂(Fur)氨基酸突变导致SodB表达降低,与甲硝唑耐药性的发生有关。3) FecA1是通过向SodB提供Fe(2+)来决定宿主定殖能力的重要决定因素,表明FecA1可能是开发新型杀菌药物的可能靶点。4)细胞内CagA癌蛋白通过自噬降解,因此寿命短。然而,在表达cd44v9的胃细胞中,CagA通过抑制自噬诱导特异性积累。
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[Study of infection strategies of Helicobacter pylori and host cell response against CagA oncoprotein].

Chronic infection with Helicobacter pylori is involved in a variety of clinical outcomes including gastric cancer. In the present study, we focused on the infection strategies of H. pylori associated with establishment of chronic infection. As a result, the following four findings revealed. 1) alpha-ketoglutarate oxidoreductase (KOR) is an essential survival enzyme for energy metabolism in the coccoid form of H. pylori, and inactivation of the KOR activity exerted a potent bactericidal action against H. pylori by preventing induction of the coccoid form. 2) SodB expression is derepressed by amino acids mutation of ferric uptake regulator (Fur), which is associated with the development of Metronidazole resistance. 3) FecA1 is an important determinant of the host-colonization ability through Fe(2+) supply to SodB, suggesting that FecA1 may be a possible target for the development of a novel bactericidal drug. 4) Intracellular CagA oncoprotein is degraded by autophagy and therefore short lived. However, in the CD44v9-expressing gastric cells, CagA specifically accumulated through the repression of autophagy induction.

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[Study on biofilm formation and heterogeneity in Clostridium perfringens]. [Wakate Colosseum for Bacteriology]. [Award Lecture]. [Workshop]. [Luncheon Seminar].
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