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多脱氧核糖核苷酸和多核糖核苷酸对大肠杆菌环磷酸腺苷受体蛋白胰蛋白酶切割的致敏作用。

Sensitization of the Escherichia coli cyclic AMP receptor protein to trypsin cleavage by polydeoxyribonucleotides and polyribonucleotides.

作者信息

Angulo J, Krakow J S

出版信息

J Biol Chem. 1986 Aug 25;261(24):11315-9.

PMID:3015965
Abstract

In the absence of cAMP the cyclic AMP receptor protein (CRP) is relatively resistant to trypsin whereas the cAMP X CRP complex is attacked yielding N-terminal core fragments of 14,300 and 18,500 Da which still bind cAMP. The DNA X CRP complex formed at low ionic strength in the absence of cAMP is cleaved by trypsin with the formation of 9,700- and 6,000-Da fragments and the concomitant loss of cAMP binding activity. DNA X CRP remains as resistant to attack by subtilisin, clostripain, and the Staphylococcus aureus V8 protease as unliganded CRP but is slowly digested by chymotrypsin. All of the double-stranded polydeoxyribonucleotides and several of the single-stranded polydeoxyribonucleotides and polyribonucleotides tested render CRP sensitive to cleavage by trypsin. CRP is less rapidly cleaved by trypsin in the presence of d(A)n, d(I)n, and r(C)n indicative of a weaker affinity of CRP for these polynucleotides. The 9,700-Da fragment is N-terminal in CRP and probably terminates at Lys-89. The loss of cAMP binding activity following trypsin cleavage of DNA X CRP indicates that regions beyond this residue are important in the function of the cAMP-binding domain of CRP. The 6,000-Da fragment extends from Val-131 to Arg-185 or Lys-188 and contains part of the F helix involved in DNA binding by CRP.

摘要

在缺乏环磷酸腺苷(cAMP)的情况下,环磷酸腺苷受体蛋白(CRP)对胰蛋白酶相对具有抗性,而cAMP与CRP的复合物则会受到攻击,产生分子量为14,300和18,500道尔顿的N端核心片段,这些片段仍能结合cAMP。在缺乏cAMP的低离子强度条件下形成的DNA与CRP复合物会被胰蛋白酶切割,形成9,700道尔顿和6,000道尔顿的片段,并伴随着cAMP结合活性的丧失。DNA与CRP复合物对枯草杆菌蛋白酶、梭菌蛋白酶和金黄色葡萄球菌V8蛋白酶的攻击仍具有抗性,如同未结合配体的CRP一样,但会被胰凝乳蛋白酶缓慢消化。所有测试的双链多脱氧核糖核苷酸以及几种单链多脱氧核糖核苷酸和多核糖核苷酸都会使CRP对胰蛋白酶切割敏感。在存在d(A)n、d(I)n和r(C)n的情况下,CRP被胰蛋白酶切割的速度较慢,这表明CRP对这些多核苷酸的亲和力较弱。9,700道尔顿的片段位于CRP的N端,可能终止于赖氨酸-89。胰蛋白酶切割DNA与CRP复合物后cAMP结合活性的丧失表明,该残基以外的区域对CRP的cAMP结合结构域的功能很重要。6,000道尔顿的片段从缬氨酸-131延伸至精氨酸-185或赖氨酸-188,包含CRP与DNA结合所涉及的F螺旋的一部分。

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