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白色念珠菌的交配型构型(a/α 对 a/a 或 α/α)导致不同途径调控的不同生物膜。

Alternative mating type configurations (a/α versus a/a or α/α) of Candida albicans result in alternative biofilms regulated by different pathways.

机构信息

Department of Biology, The University of Iowa, Iowa City, Iowa, United States of America.

出版信息

PLoS Biol. 2011 Aug;9(8):e1001117. doi: 10.1371/journal.pbio.1001117. Epub 2011 Aug 2.

Abstract

Similar multicellular structures can evolve within the same organism that may have different evolutionary histories, be controlled by different regulatory pathways, and play similar but nonidentical roles. In the human fungal pathogen Candida albicans, a quite extraordinary example of this has occurred. Depending upon the configuration of the mating type locus (a/α versus a/a or α/α), C. albicans forms alternative biofilms that appear similar morphologically, but exhibit dramatically different characteristics and are regulated by distinctly different signal transduction pathways. Biofilms formed by a/α cells are impermeable to molecules in the size range of 300 Da to 140 kDa, are poorly penetrated by human polymorphonuclear leukocytes (PMNs), and are resistant to antifungals. In contrast, a/a or α/α biofilms are permeable to molecules in this size range, are readily penetrated by PMNs, and are susceptible to antifungals. By mutational analyses, a/α biofilms are demonstrated to be regulated by the Ras1/cAMP pathway that includes Ras1→Cdc35→cAMP(Pde2-|)→Tpk2(Tpk1)→Efg1→Tec1→Bcr1, and a/a biofilms by the MAP kinase pathway that includes Mfα→Ste2→ (Ste4, Ste18, Cag1)→Ste11→Hst7→Cek2(Cek1)→Tec1. These observations suggest the hypothesis that while the upstream portion of the newly evolved pathway regulating a/a and α/α cell biofilms was derived intact from the upstream portion of the conserved pheromone-regulated pathway for mating, the downstream portion was derived through modification of the downstream portion of the conserved pathway for a/α biofilm formation. C. albicans therefore forms two alternative biofilms depending upon mating configuration.

摘要

类似的多细胞结构可以在具有不同进化历史、受不同调控途径控制且发挥相似但不同作用的同一生物体中进化。在人类真菌病原体白念珠菌中,就出现了一个非常特殊的例子。根据交配型基因座(a/α 对 a/a 或 α/α)的构型,白念珠菌形成了不同的生物膜,这些生物膜在形态上相似,但表现出截然不同的特征,并受截然不同的信号转导途径调控。a/α 细胞形成的生物膜对 300 Da 至 140 kDa 大小的分子不可渗透,不易被人类多形核白细胞(PMN)穿透,且对抗真菌药物有抗性。相比之下,a/a 或 α/α 生物膜对该大小范围内的分子是可渗透的,PMN 容易穿透,且对抗真菌药物敏感。通过突变分析,证明 a/α 生物膜由 Ras1/cAMP 途径调控,该途径包括 Ras1→Cdc35→cAMP(Pde2-|)→Tpk2(Tpk1)→Efg1→Tec1→Bcr1,而 a/a 生物膜由 MAP 激酶途径调控,该途径包括 Mfα→Ste2→(Ste4、Ste18、Cag1)→Ste11→Hst7→Cek2(Cek1)→Tec1。这些观察结果提出了一个假设,即尽管调节 a/a 和 α/α 细胞生物膜的新进化途径的上游部分完整地来自交配的保守交配型调控途径的上游部分,但下游部分是通过保守途径的下游部分的修饰而产生的,用于 a/α 生物膜的形成。因此,白念珠菌根据交配构型形成两种替代的生物膜。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/382f/3149048/b9713b3984bd/pbio.1001117.g001.jpg

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