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细菌血红蛋白受体对血红蛋白结合和血红素利用的突变分析。

Mutational analysis of hemoglobin binding and heme utilization by a bacterial hemoglobin receptor.

机构信息

Departments of Medicine.

出版信息

J Bacteriol. 2013 Jul;195(13):3115-23. doi: 10.1128/JB.00199-13. Epub 2013 May 10.

Abstract

Iron is an essential nutrient for most living organisms. To acquire iron from their environment, Gram-negative bacteria use TonB-dependent transporters that bind host proteins at the bacterial surface and transport iron or heme to the periplasm via the Ton machinery. TonB-dependent transporters are barrel-shaped outer membrane proteins with 22 transmembrane domains, 11 surface-exposed loops, and a plug domain that occludes the pore. To identify key residues of TonB-dependent transporters involved in hemoglobin binding and heme transport and thereby locate putative protective epitopes, the hemoglobin receptor of Haemophilus ducreyi HgbA was used as a model of iron/heme acquisition from hemoglobin. Although all extracellular loops of HgbA are required by H. ducreyi to use hemoglobin as a source of iron/heme, we previously demonstrated that hemoglobin binding by HgbA only involves loops 5 and 7. Using deletion, substitution, and site-directed mutagenesis, we were able to differentiate hemoglobin binding and heme acquisition by HgbA. Deletion or substitution of the GYEAYNRQWWA region of loop 5 and alanine replacement of selected histidines affected hemoglobin binding by HgbA. Conversely, mutation of the phenylalanine in the loop 7 FRAP domain or substitution of the NRQWWA motif of loop 5 significantly abrogated utilization of heme from hemoglobin. Our findings show that hemoglobin binding and heme utilization by a bacterial hemoglobin receptor involve specific motifs of HgbA.

摘要

铁是大多数生物的必需营养物质。革兰氏阴性菌使用 TonB 依赖性转运体从环境中获取铁,这些转运体与细菌表面的宿主蛋白结合,并通过 Ton 机制将铁或血红素运输到周质中。TonB 依赖性转运体是桶形的外膜蛋白,具有 22 个跨膜结构域、11 个暴露于表面的环和一个阻塞孔的塞子结构域。为了鉴定 TonB 依赖性转运体中参与血红蛋白结合和血红素转运的关键残基,从而定位潜在的保护性表位,我们使用杜氏嗜血杆菌 HgbA 的血红蛋白受体作为从血红蛋白中获取铁/血红素的模型。虽然 HgbA 的所有细胞外环都被 H. ducreyi 用来将血红蛋白作为铁/血红素的来源,但我们之前已经证明,HgbA 与血红蛋白的结合仅涉及环 5 和环 7。通过缺失、取代和定点突变,我们能够区分 HgbA 的血红蛋白结合和血红素摄取。环 5 中 GYEAYNRQWWA 区域的缺失或取代以及选定组氨酸的丙氨酸取代会影响 HgbA 的血红蛋白结合。相反,环 7 FRAP 结构域中苯丙氨酸的突变或环 5 中 NRQWWA 基序的取代会显著削弱血红蛋白中血红素的利用。我们的发现表明,细菌血红蛋白受体的血红蛋白结合和血红素利用涉及 HgbA 的特定基序。

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