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头孢烯类7α位取代对摩根氏摩根菌中β-内酰胺酶稳定性及其与青霉素结合蛋白亲和力的影响。

Effect of 7 alpha substitution of cephems on their beta-lactamase stability and affinity for penicillin-binding proteins in Morganella morganii.

作者信息

Ohya S, Yamazaki M, Sugawara S

出版信息

Antimicrob Agents Chemother. 1983 Apr;23(4):522-5. doi: 10.1128/AAC.23.4.522.

Abstract

Cephamycins, which have a methoxy group at the 7 alpha position of their cephalosporin nuclei, were highly stable against hydrolysis by a beta-lactamase purified from a clinical isolate of Morganella morganii, whereas their 7 alpha-H analogs were rapidly hydrolyzed by the enzyme. The high stability of the cephamycins was not due to their low affinity for the enzyme, since the cephamycins strongly inhibited the enzyme in a competitive manner. In cases in which the 7 alpha-methoxy group was substituted by OC2H5, SCH3, CN, or CH3 groups, the substituted compounds still showed high stability against enzymatic hydrolysis but significantly reduced both their affinities for the enzyme and their antibacterial activities. These 7 alpha-substituted cephalosporins, except for cephamycins, also had greatly reduced affinities for target proteins, i.e., penicillin-binding proteins, of beta-lactam antibiotics. Therefore, the 7 alpha position of cephalosporins was considered to play an important role in both beta-lactamase stability and antibacterial activity.

摘要

头孢霉素类抗生素在其头孢菌素核的7α位上有一个甲氧基,对从摩根氏摩根菌临床分离株中纯化得到的β-内酰胺酶的水解作用具有高度稳定性,而它们的7α-H类似物则会被该酶迅速水解。头孢霉素类抗生素的高稳定性并非因其对该酶的亲和力低,因为头孢霉素类抗生素能以竞争性方式强烈抑制该酶。当7α-甲氧基被OC2H5、SCH3、CN或CH3基团取代时,取代后的化合物对酶促水解仍表现出高稳定性,但它们对该酶的亲和力及其抗菌活性均显著降低。除头孢霉素类抗生素外,这些7α-取代的头孢菌素对β-内酰胺抗生素的靶蛋白(即青霉素结合蛋白)的亲和力也大大降低。因此,头孢菌素的7α位被认为在β-内酰胺酶稳定性和抗菌活性方面均发挥着重要作用。

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