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生长中的淋球菌释放可溶性肽聚糖:己糖胺酶和酰胺酶活性。

Release of soluble peptidoglycan from growing gonococci: hexaminidase and amidase activities.

作者信息

Rosenthal R S

出版信息

Infect Immun. 1979 Jun;24(3):869-78. doi: 10.1128/iai.24.3.869-878.1979.

Abstract

Peptidoglycan (PG) turnover in exponentially growing Neisseria gonorrhoeae RD5 type 4 was accompanied by release of soluble PG fragments into the medium. Turnover of the D-[14C]glucosamine-labeled glycan moiety and of the meso-[3H]diaminopimelic acid (DAP)-labeled peptide region occurred at similar rates (ca. 35% per generation). Turnover of D-[14C]alanine-labeled sites within the peptide side chain of PG occurred at roughly twice this rate; no turnover of L-[3H]proline-labeled protein was detected. Gel filtration of supernatants of cultures grown in the presence of labeled DAP, glucosamine, and D-alanine as described above and paper chromatography of hydrolyzed peak fractions revealed four major types of soluble PG. Two of these contained both peptide and glycan moieties and appeared to represent forms of disaccharide peptide monomers and dimers. The other two were (i) a 3H-labeled product lacking 14C and (ii) a 14C-containing product lacking 3H, which were similar in size to that expected for free tetrapeptides and free disaccharides, respectively. Together the appearance of these PG fragments and the concurrent turnover of glycan and peptide regions indicate that both glycan splitting and amidase PG hydrolase activities are involved in the turnover of PG in growing gonococci. If released during gonococcal infections, similar soluble PG fragments might influence the consequences of host-gonococcus interactions.

摘要

在指数生长的淋病奈瑟菌RD5 4型中,肽聚糖(PG)的周转伴随着可溶性PG片段释放到培养基中。D-[14C]葡萄糖胺标记的聚糖部分和内消旋-[3H]二氨基庚二酸(DAP)标记的肽区域的周转速率相似(约每代35%)。PG肽侧链中D-[14C]丙氨酸标记位点的周转速率约为此速率的两倍;未检测到L-[3H]脯氨酸标记蛋白的周转。如上所述,对在标记的DAP、葡萄糖胺和D-丙氨酸存在下培养的上清液进行凝胶过滤,并对水解后的峰馏分进行纸色谱分析,发现了四种主要类型的可溶性PG。其中两种同时含有肽和聚糖部分,似乎代表二糖肽单体和二聚体的形式。另外两种是(i)一种缺乏14C的3H标记产物和(ii)一种缺乏3H的含14C产物,其大小分别与游离四肽和游离二糖的预期大小相似。这些PG片段的出现以及聚糖和肽区域的同时周转表明,聚糖裂解和酰胺酶PG水解酶活性都参与了生长中的淋球菌中PG的周转。如果在淋球菌感染期间释放,类似的可溶性PG片段可能会影响宿主-淋球菌相互作用的结果。

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