Institute of Agrochemistry and Food Technology, Microbiome, Nutrition and Health Research Unit, Spanish National Research Council, IATA-CSIC, 46980, Paterna-Valencia, Spain.
Principe Felipe Research Center (CIPF), Host-Microbe Interactions in Metabolic Health Laboratory, 46012, Valencia, Spain.
Genome Biol. 2024 Jul 3;25(1):174. doi: 10.1186/s13059-024-03325-4.
The gut microbiota controls broad aspects of human metabolism and feeding behavior, but the basis for this control remains largely unclear. Given the key role of human dipeptidyl peptidase 4 (DPP4) in host metabolism, we investigate whether microbiota DPP4-like counterparts perform the same function.
We identify novel functional homologs of human DPP4 in several bacterial species inhabiting the human gut, and specific associations between Parabacteroides and Porphyromonas DPP4-like genes and type 2 diabetes (T2D). We also find that the DPP4-like enzyme from the gut symbiont Parabacteroides merdae mimics the proteolytic activity of the human enzyme on peptide YY, neuropeptide Y, gastric inhibitory polypeptide (GIP), and glucagon-like peptide 1 (GLP-1) hormones in vitro. Importantly, administration of E. coli overexpressing the P. merdae DPP4-like enzyme to lipopolysaccharide-treated mice with impaired gut barrier function reduces active GIP and GLP-1 levels, which is attributed to increased DPP4 activity in the portal circulation and the cecal content. Finally, we observe that linagliptin, saxagliptin, sitagliptin, and vildagliptin, antidiabetic drugs with DPP4 inhibitory activity, differentially inhibit the activity of the DPP4-like enzyme from P. merdae.
Our findings confirm that proteolytic enzymes produced by the gut microbiota are likely to contribute to the glucose metabolic dysfunction that underlies T2D by inactivating incretins, which might inspire the development of improved antidiabetic therapies.
肠道微生物群控制着人类代谢和进食行为的广泛方面,但这种控制的基础在很大程度上仍不清楚。鉴于人类二肽基肽酶 4(DPP4)在宿主代谢中的关键作用,我们研究了微生物群 DPP4 样对应物是否执行相同的功能。
我们在几种栖息在人类肠道中的细菌物种中鉴定出人类 DPP4 的新型功能同源物,并且 Parabacteroides 和 Porphyromonas DPP4 样基因与 2 型糖尿病(T2D)之间存在特定关联。我们还发现,来自肠道共生菌 Parabacteroides merdae 的 DPP4 样酶在体外模拟了人类酶对肽 YY、神经肽 Y、胃抑制多肽(GIP)和胰高血糖素样肽 1(GLP-1)激素的蛋白水解活性。重要的是,向肠道屏障功能受损的脂多糖处理小鼠施用过度表达 P. merdae DPP4 样酶的大肠杆菌会降低活性 GIP 和 GLP-1 水平,这归因于门脉循环和盲肠内容物中 DPP4 活性的增加。最后,我们观察到,具有 DPP4 抑制活性的抗糖尿病药物利拉利汀、沙格列汀、西他列汀和维格列汀,可不同程度地抑制 P. merdae 的 DPP4 样酶的活性。
我们的发现证实,肠道微生物群产生的蛋白水解酶可能通过使肠降血糖素失活而导致 2 型糖尿病的葡萄糖代谢功能障碍,这可能激发更好的抗糖尿病疗法的发展。
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