酿酒酵母在高温胁迫下的存活需要CCT和细胞壁完整性通路之间的通信。

IF 1.8 4区 生物学 Q3 BIOLOGY Biologia futura Pub Date : 2023-12-01 Epub Date: 2023-11-15 DOI:10.1007/s42977-023-00192-1
Ankita Dube, Dileep Pullepu, M Anaul Kabir
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引用次数: 0

摘要

伴侣蛋白TRiC/CCT是由8个必需基因CCT1-8编码的16个亚基的细胞质圆柱形复合体。它有助于折叠酵母中10%的细胞多肽。在Cct7p的赤道结构域携带G412E取代点突变的菌株导致底物折叠不当。在这项研究中,Cct7p突变体对非最佳生长温度和细胞壁应激源表现出敏感性。众所周知,热休克会破坏出芽酵母的细胞壁和蛋白质稳定性。丝裂原活化蛋白激酶介导的细胞壁完整性通路被激活以补偿受到干扰的细胞壁。突变体中MAPK信号通路PKC1和SLT2基因的过表达挽救了生长和细胞分裂缺陷。此外,CWI通路的SED1、GFA1、PIR1、RIM21等基因下调。Cct7p突变株(G412E)由于蛋白质折叠和细胞壁维持的潜在缺陷而无法承受热应激。综上所述,我们的结果强烈表明CCT与细胞壁完整性途径之间的相互作用。
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Saccharomyces cerevisiae survival against heat stress entails a communication between CCT and cell wall integrity pathway.

The chaperonin TRiC/CCT is cytosolic cylindrical complex of 16 subunits encoded by eight essential genes CCT1-8. It contributes to folding 10% of cellular polypeptides in yeast. The strain carrying substitution point mutation G412E in the equatorial domain of Cct7p resulted in the improper folding of substrates. In this study, the Cct7p mutant exhibited sensitivity to non-optimal growth temperatures and cell wall stressors. Heat shock is known to disrupt cell wall and protein stability in budding yeast. Mitogen-activated protein kinase-mediated cell wall integrity pathway gets activated to compensate the perturbed cell wall. Overexpression of the PKC1 and SLT2 genes of MAPK signaling pathway in mutant rescued the growth and cell division defects. Additionally, the genes of the CWI pathway such as SED1, GFA1, PIR1, and RIM21 are down-regulated. The Cct7p mutant strain (G412E) is unable to withstand the heat stress due to the underlying defects in protein folding and cell wall maintenance. Taken together, our results strongly indicate the interaction between CCT and cell wall integrity pathway.

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来源期刊
Biologia futura
Biologia futura Agricultural and Biological Sciences-Agricultural and Biological Sciences (all)
CiteScore
3.50
自引率
0.00%
发文量
27
期刊介绍: How can the scientific knowledge we possess now influence that future? That is, the FUTURE of Earth and life − of humankind. Can we make choices in the present to change our future? How can 21st century biological research ask proper scientific questions and find solid answers? Addressing these questions is the main goal of Biologia Futura (formerly Acta Biologica Hungarica). In keeping with the name, the new mission is to focus on areas of biology where major advances are to be expected, areas of biology with strong inter-disciplinary connection and to provide new avenues for future research in biology. Biologia Futura aims to publish articles from all fields of biology.
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