腱鞘蛋白的演变

Josephine C. Adams, Richard P. Tucker
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摘要

背景细胞外基质的进化与元古宙器官发生的进化密切相关。腱鞘蛋白是脊索动物的细胞外基质糖蛋白,参与整合素信号转导和形态发生。无脊椎脊索动物编码单个腱鞘蛋白,脊椎动物中发现多个腱鞘蛋白旁系亲属(被命名为腱鞘蛋白-C、腱鞘蛋白-R、腱鞘蛋白-W和腱鞘蛋白-X),但总体而言,该家族的进化过程仍不清楚。结果 本研究考察了半脊索动物、头脊索动物、鳞栉水母纲动物、无颌类动物、软骨鱼类、叶鳍鱼类、鳐鳍鱼类和代表性四足动物的基因组,以鉴定预测的腱鞘蛋白。我们通过序列保持、分子系统发育和编码基因的同源保守性研究,全面评估了它们之间的进化关系。由此产生的新进化模型假设腱鞘蛋白起源于脊索动物的祖先,在脊椎动物的祖先发生全基因组复制事件之后,出现了腱鞘蛋白-C和腱鞘蛋白-R的类似旁系亲属。tenascin-X是在祖先地龙类的第二轮全基因组复制后出现的,很可能是编码tenascin-R同源物的基因复制产生的。第四个基因编码 tenascin-W(也称为 tenascin-N),显然是由 tenascin-R 的局部复制产生的。结论 在无颌类和地龙中观察到的 tenascin 同源物的多样性是通过选择性保留新基因进化而来的,这些新基因是由全基因组和局部复制事件共同产生的。特异性tenascin旁系亲属的进化出现与脊椎动物特异性细胞和组织类型的出现相吻合,在这些细胞和组织类型中,tenascin旁系亲属被大量表达,例如颅内和面部骨骼(tenascin-C)、扩展的中枢神经系统(tenascin-R)和骨骼(tenascin-W)。
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The evolution of tenascins

Background

The evolution of extracellular matrix is tightly linked to the evolution of organogenesis in metazoans. Tenascins are extracellular matrix glycoproteins of chordates that participate in integrin-signaling and morphogenetic events. Single tenascins are encoded by invertebrate chordates, and multiple tenascin paralogs are found in vertebrates (designated tenascin-C, tenascin-R, tenascin-W and tenascin-X) yet, overall, the evolution of this family has remained unclear.

Results

This study examines the genomes of hemichordates, cephalochordates, tunicates, agnathans, cartilaginous fishes, lobe-finned fishes, ray-finned fishes and representative tetrapods to identify predicted tenascin proteins. We comprehensively assess their evolutionary relationships by sequence conservation, molecular phylogeny and examination of conservation of synteny of the encoding genes. The resulting new evolutionary model posits the origin of tenascin in an ancestral chordate, with tenascin-C-like and tenascin-R-like paralogs emerging after a whole genome duplication event in an ancestral vertebrate. Tenascin-X appeared following a second round of whole genome duplication in an ancestral gnathostome, most likely from duplication of the gene encoding the tenascin-R homolog. The fourth gene, encoding tenascin-W (also known as tenascin-N), apparently arose from a local duplication of tenascin-R.

Conclusions

The diversity of tenascin paralogs observed in agnathans and gnathostomes has evolved through selective retention of novel genes that arose from a combination of whole genome and local duplication events. The evolutionary appearance of specific tenascin paralogs coincides with the appearance of vertebrate-specific cell and tissue types where the paralogs are abundantly expressed, such as the endocranium and facial skeleton (tenascin-C), an expanded central nervous system (tenascin-R), and bone (tenascin-W).

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