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肌生成抑制蛋白是一种促纤维化因子,也是横纹肌质量的主要抑制剂,存在于阴茎和血管平滑肌中。

Myostatin, a profibrotic factor and the main inhibitor of striated muscle mass, is present in the penile and vascular smooth muscle.

作者信息

Kovanecz I, Masouminia M, Gelfand R, Vernet D, Rajfer J, Gonzalez-Cadavid N F

机构信息

Division of Urology, Department of Surgery, Los Angeles Biomedical Research Institute at Harbor-UCLA Medical Center, Torrance, CA, USA.

Department of Urology, David Geffen School of Medicine at UCLA, Los Angeles, CA, USA.

出版信息

Int J Impot Res. 2017 Sep;29(5):194-201. doi: 10.1038/ijir.2017.22. Epub 2017 May 25.

Abstract

Myostatin is present in striated myofibers but, except for myometrial cells, has not been reported within smooth muscle cells (SMC). We investigated in the rat whether myostatin is present in SMC within the penis and the vascular wall and, if so, whether it is transcriptionally expressed and associated with the loss of corporal SMC occurring in certain forms of erectile dysfunction (ED). Myostatin protein was detected by immunohistochemistry/fluorescence and western blots in the perineal striated muscles, and also in the SMC of the penile corpora, arteries and veins, and aorta. Myostatin was found in corporal SMC cultures, and its transcriptional expression (and its receptor) was shown there by DNA microarrays. Myostatin protein was measured by western blots in the penile shaft of rats subjected to bilateral cavernosal nerve resection (BCNR), that were left untreated, or treated (45 days) with muscle-derived stem cells (MDSC), or concurrent daily low-dose sildenafil. Myostatin was not increased by BCNR (compared with sham operated animals), but over expressed after treatment with MDSC. This was reduced by concurrent sildenafil. The presence of myostatin in corporal and vascular SMC, and its overexpression in the corpora by MDSC therapy, may have relevance for the stem cell treatment of corporal fibrosis and ED.

摘要

肌生成抑制蛋白存在于横纹肌纤维中,但除子宫肌层细胞外,尚未见其在平滑肌细胞(SMC)中的报道。我们在大鼠中研究了阴茎和血管壁的SMC中是否存在肌生成抑制蛋白,若存在,其是否转录表达以及是否与某些形式勃起功能障碍(ED)中海绵体SMC的丧失有关。通过免疫组织化学/荧光和蛋白质印迹法在会阴横纹肌以及阴茎海绵体、动脉、静脉和主动脉的SMC中检测到了肌生成抑制蛋白。在海绵体SMC培养物中发现了肌生成抑制蛋白,并通过DNA微阵列显示了其转录表达(及其受体)。通过蛋白质印迹法测定了双侧海绵体神经切除(BCNR)大鼠阴茎体中的肌生成抑制蛋白,这些大鼠未接受治疗、接受(45天)肌肉衍生干细胞(MDSC)治疗或同时每日给予低剂量西地那非。BCNR(与假手术动物相比)未使肌生成抑制蛋白增加,但MDSC治疗后其表达上调。同时使用西地那非可使其降低。海绵体和血管SMC中肌生成抑制蛋白的存在及其通过MDSC疗法在海绵体中的过表达,可能与海绵体纤维化和ED的干细胞治疗有关。

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