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对[具体研究对象]中磺糖酵解的研究揭示了二羟基丙烷磺酸盐降解的一种广泛存在的分支途径。

Study of sulfoglycolysis in reveals a widespread bifurcated pathway for dihydroxypropanesulfonate degradation.

作者信息

Chen Yiwei, Chu Ruoxing, Ma Kailiang, Jiang Li, Yang Qiaoyu, Li Zhi, Hu Min, Guo Qiuyi, Lu Fengxia, Wei Yifeng, Zhang Yan, Tong Yang

机构信息

College of Food Science and Technology, Nanjing Agricultural University, Nanjing 210095, China.

New Cornerstone Science Laboratory, School of Pharmaceutical Science and Technology, Tianjin University, Tianjin 300072, China.

出版信息

iScience. 2024 Sep 21;27(10):111010. doi: 10.1016/j.isci.2024.111010. eCollection 2024 Oct 18.

Abstract

Sulfoquinovose (SQ), the polar head group of sulfolipids essential for photosynthesis, is naturally abundant. Anaerobic Firmicutes degrade SQ through a transaldolase-dependent (sulfo-TAL) pathway, producing dihydroxypropanesulfonate (DHPS). Some bacteria extend this pathway by the sequential action of HpfG and HpfD converting DHPS to 3-hydroxypropanesulfonate (3-HPS) via 3-sulfopropionaldehyde (3-SPA). Here, we report a variant sulfo-TAL pathway in , involving additional enzymes, a NAD-dependent 3-SPA dehydrogenase HpfX, and a 3-sulfopropionyl-CoA synthetase HpfYZ, which oxidize 3-SPA to 3-sulfopropionate (3-SP) coupled with ATP formation. grown on SQ or DHPS produced a mixture of 3-HPS and 3-SP, indicating the bifurcated pathway. Similar genes are found in various Firmicutes, including gut bacteria. Importantly, 3-SP, but not 3-HPS, can serve as a respiratory terminal electron acceptor for , a common intestinal pathobiont, resulting in the production of toxic HS. This research expands our understanding of sulfonate metabolism and reveals cross-feeding in the anaerobic microbiome.

摘要

磺基喹诺糖(SQ)是光合作用所必需的硫脂的极性头部基团,在自然界中含量丰富。厌氧厚壁菌通过一条依赖转醛醇酶的(磺基 - TAL)途径降解SQ,产生二羟基丙烷磺酸盐(DHPS)。一些细菌通过HpfG和HpfD的相继作用扩展这条途径,将DHPS经由3 - 磺基丙醛(3 - SPA)转化为3 - 羟基丙烷磺酸盐(3 - HPS)。在此,我们报道了一种存在于[具体细菌名称未给出]中的变异磺基 - TAL途径,该途径涉及额外的酶,一种依赖NAD的3 - SPA脱氢酶HpfX和一种3 - 磺基丙酰 - CoA合成酶HpfYZ,它们将3 - SPA氧化为3 - 磺基丙酸(3 - SP)并伴随ATP形成。在SQ或DHPS上生长的[具体细菌名称未给出]产生了3 - HPS和3 - SP的混合物,表明存在分支途径。在包括肠道细菌在内的各种厚壁菌中都发现了类似的基因。重要的是,3 - SP而非3 - HPS可以作为常见肠道病原菌[具体细菌名称未给出]的呼吸末端电子受体,导致产生有毒的HS。这项研究扩展了我们对磺酸盐代谢的理解,并揭示了厌氧微生物群落中的交叉营养现象。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/2939/11489063/db483b81706e/fx1.jpg

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