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小窝蛋白-1α和-1β在脊椎动物早期发育中发挥非冗余作用。

Caveolin-1alpha and -1beta perform nonredundant roles in early vertebrate development.

作者信息

Fang Ping-Ke, Solomon Keith R, Zhuang Liyan, Qi Maosong, McKee Mary, Freeman Michael R, Yelick Pamela C

机构信息

Urological Diseases Research Center, Department of Orthopaedic Surgery, Children's Hospital Boston, Harvard Medical School, Enders Research Laboratories, Suite 1161, 300 Longwood Ave., Boston, MA 02115, USA.

出版信息

Am J Pathol. 2006 Dec;169(6):2209-22. doi: 10.2353/ajpath.2006.060562.

Abstract

Caveolins are integral membrane proteins that localize predominantly to lipid rafts, where they oligomerize to form flask-shaped organelles termed caveolae and play important roles in membrane trafficking, signal transduction, and other cellular processes. To investigate potential roles for caveolin-1 (cav-1) in development, cav-1alpha and -1beta cDNAs were functionally characterized in the zebrafish. Cav-1alpha and -1beta mRNAs exhibited overlapping but distinct expression patterns throughout embryogenesis. Targeted depletion of either Cav-1 isoform, using antisense morpholino oligomers, resulted in a substantial loss of caveolae and dramatic neural, eye, and somite defects by 12 hours after fertilization, the time at which mRNA levels of both isoforms substantially increased in wild-type animals. Morphant phenotypes were rescued by injection of homotypic (cav-1alpha/cav-1alpha) but not heterotypic (cav-1alpha/cav-1beta) zebrafish and human cav-1 cRNAs, revealing nonredundant and evolutionarily conserved functions for the individual Cav-1 isoforms. Mutation of a known Cav-1 phosphorylation site unique to Cav-1alpha (Y14-->F) resulted in a failure to rescue the cav-1alpha morphant phenotype, verifying an essential role for Cav-1alpha specifically and implicating this residue in early developmental functions. Cav-1alpha and -1beta morphants also exhibited disruption in the actin cytoskeleton. These results support important and previously unanticipated roles for the Caveolin-1 isoforms in vertebrate organogenesis.

摘要

小窝蛋白是整合膜蛋白,主要定位于脂筏,在那里它们寡聚形成称为小窝的烧瓶状细胞器,并在膜运输、信号转导和其他细胞过程中发挥重要作用。为了研究小窝蛋白-1(cav-1)在发育中的潜在作用,在斑马鱼中对cav-1α和-1β cDNA进行了功能表征。在整个胚胎发育过程中,Cav-1α和-1β mRNA表现出重叠但不同的表达模式。使用反义吗啉代寡聚物靶向耗尽任何一种Cav-1亚型,在受精后12小时导致小窝大量丧失以及明显的神经、眼睛和体节缺陷,此时两种亚型的mRNA水平在野生型动物中大幅增加。通过注射同型(cav-1α/cav-1α)而非异型(cav-1α/cav-1β)斑马鱼和人类cav-1 cRNA挽救了突变体表型,揭示了单个Cav-1亚型的非冗余和进化保守功能。对Cav-1α特有的已知Cav-1磷酸化位点(Y14→F)进行突变导致无法挽救cav-1α突变体表型,证实了Cav-1α的特定重要作用,并暗示该残基在早期发育功能中的作用。Cav-1α和-1β突变体还表现出肌动蛋白细胞骨架的破坏。这些结果支持了小窝蛋白-1亚型在脊椎动物器官发生中的重要且先前未预料到的作用。

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