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色氨酸代谢物图谱揭示了器官、年龄和性别特异性差异。

Tryptophan metabolite atlas uncovers organ, age, and sex-specific variations.

作者信息

Perez-Castro Lizbeth, Nawas Afshan F, Kilgore Jessica A, Nogueira Pedro A S, Lafita-Navarro M Carmen, Acosta Paul H, Garcia Roy, Williams Noelle S, Conacci-Sorrell Maralice

机构信息

Department of Cell Biology, University of Texas Southwestern Medical Center, Dallas, USA.

Department of Biochemistry, University of Texas Southwestern Medical Center, Dallas, USA.

出版信息

FEBS Open Bio. 2025 Sep 19. doi: 10.1002/2211-5463.70123.

Abstract

Tryptophan (Trp) is the largest and most structurally complex amino acid, yet it is the least abundant in the proteome. Its distinct indole ring and high carbon content allow it to give rise to several biologically active metabolites, including serotonin, kynurenine (Kyn), and indole-3-pyruvate (I3P). Dysregulation of Trp metabolism has been implicated in a range of diseases, from depression to cancer. Investigating Trp and its metabolites in healthy tissues provides insight into how disease-associated disruptions may be targeted selectively while preserving essential physiological functions. Whereas previous studies have typically focused on individual organs or single metabolic branches, our analysis spans 12 peripheral organs, the central nervous system, and serum in male and female (C57BL/6) mice across three life stages: young (3 weeks), adult (54 weeks), and aged (74 weeks). We identified striking tissue-, sex-, and age-specific differences in Trp metabolism, including elevated levels of I3P and Kyn, both linked to tumor growth, in aging males. We also compared Trp metabolite profiles in tissues from mice fed a control defined diet versus a Trp-deficient diet for three weeks. This intervention led to a marked reduction in circulating Trp and its metabolites, with more modest effects observed in the liver and central nervous system. These findings underscore the importance of organ-specific and diet-sensitive analyses of Trp metabolism for understanding its role in both normal physiology and disease. Establishing baseline levels of Trp metabolites across tissues may also provide a foundation for identifying organ-specific metabolic reprogramming in cancer and other illnesses.

摘要

色氨酸(Trp)是最大且结构最复杂的氨基酸,但在蛋白质组中含量最少。其独特的吲哚环和高碳含量使其能够产生多种生物活性代谢产物,包括血清素、犬尿氨酸(Kyn)和吲哚 - 3 - 丙酮酸(I3P)。色氨酸代谢失调与一系列疾病有关,从抑郁症到癌症。研究健康组织中的色氨酸及其代谢产物有助于深入了解如何在保留基本生理功能的同时选择性地针对与疾病相关的干扰。以往的研究通常集中在单个器官或单一代谢分支,而我们的分析涵盖了12个外周器官、中枢神经系统以及雄性和雌性(C57BL/6)小鼠在三个生命阶段(幼年(3周)、成年(54周)和老年(74周))的血清。我们发现色氨酸代谢存在显著的组织、性别和年龄特异性差异,包括老年雄性小鼠中与肿瘤生长相关的I3P和Kyn水平升高。我们还比较了喂食对照定义饮食与色氨酸缺乏饮食三周的小鼠组织中的色氨酸代谢物谱。这种干预导致循环色氨酸及其代谢产物显著减少,在肝脏和中枢神经系统中观察到的影响较小。这些发现强调了对色氨酸代谢进行器官特异性和饮食敏感性分析对于理解其在正常生理和疾病中的作用的重要性。确定各组织中色氨酸代谢物的基线水平也可能为识别癌症和其他疾病中器官特异性的代谢重编程提供基础。

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