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调控由肢体快、慢运动神经支配的猫颞肌再生中具有颌特异性的肌球蛋白结合蛋白-C 和原肌球蛋白同工型。

Regulation of jaw-specific isoforms of myosin-binding protein-C and tropomyosin in regenerating cat temporalis muscle innervated by limb fast and slow motor nerves.

机构信息

Discipline of Physiology, Building F13, Sydney Medical School, The University of Sydney, Sydney, Australia.

出版信息

J Histochem Cytochem. 2010 Nov;58(11):989-1004. doi: 10.1369/jhc.2010.956847. Epub 2010 Aug 2.

Abstract

Cat jaw-closing muscles are a distinct muscle allotype characterized by the expression of masticatory-specific myofibrillar proteins. Transplantation studies showed that expression of masticatory myosin heavy chain (m-MyHC) is promoted by fast motor nerves, but suppressed by slow motor nerves. We investigated whether masticatory myosin-binding protein-C (m-MBP-C) and masticatory tropomyosin (m-Tm) are similarly regulated. Temporalis muscle strips were transplanted into limb muscle beds to allow innervation by fast or slow muscle nerve during regeneration. Regenerated muscles were examined postoperatively up to 168 days by peroxidase IHC using monoclonal antibodies to m-MyHC, m-MBP-C, and m-Tm. Regenerates in both muscle beds expressed fetal and slow MyHCs, m-MyHC, m-MBP-C, and m-Tm during the first 4 weeks. Longer-term regenerates innervated by fast nerve suppressed fetal and slow MyHCs, retaining m-MyHC, m-MBP-C, and m-Tm, whereas fibers innervated by slow nerve suppressed fetal MyHCs and the three masticatory-specific proteins, induced slow MyHC, and showed immunohistochemical characteristics of jaw-slow fibers. We concluded that expression of m-MBP-C and m-Tm is coregulated by m-MyHC and that neural impulses to limb slow muscle are capable of suppressing masticatory-specific proteins and to channel gene expression along the jaw-slow phenotype unique to jaw-closing muscle.

摘要

猫的闭口肌肉是一种独特的肌肉同种型,其特征是表达咀嚼特异性肌球蛋白重链(m-MyHC)。移植研究表明,咀嚼型肌球蛋白重链(m-MyHC)的表达受快肌运动神经的促进,而受慢肌运动神经的抑制。我们研究了咀嚼型肌球蛋白结合蛋白-C(m-MBP-C)和咀嚼型原肌球蛋白(m-Tm)是否受到类似的调节。将颞肌条带移植到肢体肌肉床中,在再生过程中允许快肌或慢肌神经支配。术后用抗 m-MyHC、m-MBP-C 和 m-Tm 的单克隆抗体通过过氧化物酶免疫组化检查肌肉再生,直至 168 天。在两种肌肉床中,再生肌肉在最初的 4 周内表达胎儿型和慢型 MyHC、m-MyHC、m-MBP-C 和 m-Tm。由快神经支配的长期再生肌肉抑制了胎儿型和慢型 MyHC,但保留了 m-MyHC、m-MBP-C 和 m-Tm,而由慢神经支配的纤维抑制了胎儿型 MyHC 和三种咀嚼特异性蛋白,诱导了慢型 MyHC,并显示出与咀嚼肌慢纤维相关的免疫组织化学特征。我们的结论是,m-MBP-C 和 m-Tm 的表达与 m-MyHC 共同调节,肢体慢肌的神经冲动能够抑制咀嚼特异性蛋白,并沿着咀嚼肌特有的咀嚼肌慢表型引导基因表达。

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