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甲状腺功能亢进兔的主动脉内膜增厚及肌球蛋白同工型表达

Aortic intimal thickening and myosin isoform expression in hyperthyroid rabbits.

作者信息

Giuriato L, Borrione A C, Zanellato A M, Tonello M, Scatena M, Scannapieco G, Pauletto P, Sartore S

机构信息

Institute of General Pathology, University of Padova, Italy.

出版信息

Arterioscler Thromb. 1991 Sep-Oct;11(5):1376-89. doi: 10.1161/01.atv.11.5.1376.

Abstract

The potential effect of thyroid hormones on the expression of cytoskeletal and cytocontractile proteins of vascular smooth muscle cells (SMCs) was examined by a panel of monoclonal antibodies and immunocytochemical procedures. L-Thyroxine was administered to adult New Zealand White rabbits for as long as 26 days, and the aortic SMC composition was studied at days 1, 2, 7, 15, and 26 from the beginning of hormonal treatment. A diffuse intimal thickening of the aorta became visible after 7 days of thyroxine administration. Histological and histochemical examination of intimal tissues from hyperthyroid rabbits revealed the presence of a homogeneous Sudan black-negative cell population. In immunofluorescence tests the intimal cells were found to be negative for antibodies specific for monocyte/macrophage or desmin and homogenously reactive (positive) for antibodies to vimentin and smooth muscle (SM) alpha-actin, thus indicating that cells present in the thickened intima were of the SM type. In addition, intimal SMCs from aortas of hyperthyroid rabbits showed a myosin isoform content similar to that found in normal developing aortic SM and in a specific medial SMC subpopulation of aortas from adult euthyroid animals. In the media underlying the intimal thickening, almost all the SMCs switched their myosin isoform expression toward the "immature" phenotype after 2 days of thyroxine treatment. When the level of thyroid hormones was reduced by propylthiouracil treatment, the medial SMC subpopulation with the immature myosin isoform content present in euthyroid rabbits completely disappeared. The study of DNA synthesis-related bromodeoxyuridine incorporation in aortas from hyperthyroid rabbits showed the presence of labeled nuclei in medial SMCs before the appearance of the intimal thickening as well as in the thickened intima and in the underlying media at days 7 and 15. These results are consistent with a specific role for thyroid hormones in inducing proliferation/migration of medial SMCs into the intima. Moreover, the switch in the expression of myosin isoforms induced by thyroid hormones appears to precede the accumulation of medial SMCs in the intima.

摘要

通过一组单克隆抗体和免疫细胞化学方法,研究了甲状腺激素对血管平滑肌细胞(SMC)细胞骨架和细胞收缩蛋白表达的潜在影响。将L-甲状腺素给予成年新西兰白兔长达26天,并在激素治疗开始后的第1、2、7、15和26天研究主动脉SMC组成。甲状腺素给药7天后,主动脉出现弥漫性内膜增厚。对甲状腺功能亢进兔子的内膜组织进行组织学和组织化学检查,发现存在均匀的苏丹黑阴性细胞群。在免疫荧光试验中,内膜细胞对单核细胞/巨噬细胞或结蛋白特异性抗体呈阴性,对波形蛋白和平滑肌(SM)α-肌动蛋白抗体呈均匀反应(阳性),这表明增厚内膜中的细胞为SM型。此外,甲状腺功能亢进兔子主动脉的内膜SMC显示出与正常发育的主动脉SM以及成年甲状腺功能正常动物主动脉特定中膜SMC亚群中发现的肌球蛋白同工型含量相似。在内膜增厚下方的中膜中,甲状腺素治疗2天后,几乎所有SMC将其肌球蛋白同工型表达转向“不成熟”表型。当通过丙硫氧嘧啶治疗降低甲状腺激素水平时,甲状腺功能正常兔子中存在的具有不成熟肌球蛋白同工型含量的中膜SMC亚群完全消失。对甲状腺功能亢进兔子主动脉中与DNA合成相关的溴脱氧尿苷掺入的研究表明,在内膜增厚出现之前,中膜SMC中存在标记核,在第7天和第15天,增厚的内膜和下方的中膜中也存在标记核。这些结果与甲状腺激素在诱导中膜SMC增殖/迁移到内膜中的特定作用一致。此外,甲状腺激素诱导的肌球蛋白同工型表达的转变似乎先于中膜SMC在内膜中的积累。

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