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阿耳忒弥斯的金属β-内酰胺酶/β-CASP结构域构成V(D)J重组的催化核心。

The metallo-beta-lactamase/beta-CASP domain of Artemis constitutes the catalytic core for V(D)J recombination.

作者信息

Poinsignon Catherine, Moshous Despina, Callebaut Isabelle, de Chasseval Régina, Villey Isabelle, de Villartay Jean-Pierre

机构信息

Développement Normal et Pathologique de Système Immunitaire, INSERM U429, Hôpital Necker Enfants Malades, 75015 Paris, France.

出版信息

J Exp Med. 2004 Feb 2;199(3):315-21. doi: 10.1084/jem.20031142. Epub 2004 Jan 26.

Abstract

The V(D)J recombination/DNA repair factor Artemis belongs to the metallo-beta-lactamase (beta-Lact) superfamily of enzymes. Three regions can be defined within the Artemis protein sequence: (a) the beta-Lact homology domain, to which is appended (b) the beta-CASP region, specific of members of the beta-Lact superfamily acting on nucleic acids, and (c) the COOH-terminal domain. Using in vitro mutagenesis, here we show that the association of the beta-Lact and the beta-CASP regions suffices for in vivo V(D)J recombination of chromosome-integrated substrates. Single amino acid mutants point to critical catalytic residues for V(D)J recombination activity. The results presented here define the beta-Lact/beta-CASP domain of Artemis as the minimal core catalytic domain needed for V(D)J recombination and suggest that Artemis uses one or two Zn(II) ions to exert its catalytic activity, like bacterial class B beta-Lact enzymes hydrolyzing beta-lactam compounds.

摘要

V(D)J重组/DNA修复因子阿耳忒弥斯(Artemis)属于金属β-内酰胺酶(β-Lact)超家族的酶。在阿耳忒弥斯蛋白序列中可定义三个区域:(a)β-Lact同源结构域,其上附加有(b)β-CASP区域,这是作用于核酸的β-Lact超家族成员所特有的,以及(c)羧基末端结构域。通过体外诱变,我们在此表明β-Lact和β-CASP区域的结合足以实现染色体整合底物的体内V(D)J重组。单氨基酸突变体指出了V(D)J重组活性的关键催化残基。此处给出的结果将阿耳忒弥斯的β-Lact/β-CASP结构域定义为V(D)J重组所需的最小核心催化结构域,并表明阿耳忒弥斯像水解β-内酰胺化合物的细菌B类β-Lact酶一样,使用一个或两个锌(II)离子来发挥其催化活性。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/5790/2211804/169034754b59/20031142f1.jpg

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