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在现代人类进化过程中,腺苷酸琥珀酸裂解酶的活性和表达降低,影响大脑和行为。

The activity and expression of adenylosuccinate lyase were reduced during modern human evolution, affecting brain and behavior.

作者信息

Ju Xiang-Chun, Lee Shin-Yu, Ågren Richard, Machado Luiz Carlos, Xing Jiawei, Azama Chika, Roy Michael C, Endo Toshihiro, Huttner Wieland, Siepel Adam, Fukunaga Izumi, Zeberg Hugo, Pääbo Svante

机构信息

Okinawa Institute of Science and Technology Graduate University, Okinawa 904-0495, Japan.

Department of Physiology and Pharmacology, Karolinska Institutet, Stockholm 17177, Sweden.

出版信息

Proc Natl Acad Sci U S A. 2025 Aug 12;122(32):e2508540122. doi: 10.1073/pnas.2508540122. Epub 2025 Aug 4.

Abstract

Adenylosuccinate lyase (ADSL), an enzyme that is crucial for purine biosynthesis, carries an amino acid substitution that is present in almost all humans today but absent in Neandertals and Denisovans. This substitution reduces the stability of the enzyme, but what functional consequences it has are unknown. Here, we show that when introduced into mice, this substitution causes substrates of the enzyme to accumulate in amounts that correlate negatively with ADSL expression levels. In the brain, where the expression of the enzyme is low, the substitution results in particularly high substrate levels. When the behavior of the mice is analyzed, female mice expressing the modern human-like version of ADSL access water more efficiently for drinking than their wild-type littermates. In addition to the amino acid substitution, a haplotype in the ADSL gene occurs at a carrier frequency of >97% in present-day humans and exhibits evidence of positive selection. It is associated with less ADSL expression as well as with increased concentrations of succinyladenosine, one of the substrates of the enzyme, in cerebrospinal fluid. Thus, two genetic changes have reduced ADSL activity in human tissues since modern and archaic humans separated, affecting purine biosynthesis, particularly in the brain.

摘要

腺苷酸琥珀酸裂解酶(ADSL)是嘌呤生物合成过程中的一种关键酶,其携带的一个氨基酸替换几乎存在于当今所有人类中,但在尼安德特人和丹尼索瓦人中却不存在。这种替换降低了该酶的稳定性,但其功能后果尚不清楚。在此,我们表明,当将这种替换引入小鼠体内时,该酶的底物会以与ADSL表达水平呈负相关的量积累。在该酶表达较低的大脑中,这种替换导致底物水平特别高。当分析小鼠的行为时,表达现代人类样ADSL版本的雌性小鼠比其野生型同窝小鼠更有效地获取水用于饮用。除了这种氨基酸替换外,ADSL基因中的一种单倍型在当今人类中的携带频率>97%,并表现出正选择的证据。它与较低的ADSL表达以及脑脊液中该酶的一种底物琥珀酰腺苷浓度升高有关。因此,自现代人类和古代人类分离以来,两种基因变化降低了人体组织中的ADSL活性,影响了嘌呤生物合成,尤其是在大脑中。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/a334/12358879/011ac29b9b91/pnas.2508540122fig01.jpg

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