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基于细胞外基质特定化合物的子宫平滑肌瘤分子特征

[Molecular characteristics of leiomyoma uteri based on selected compounds of the extracellular matrix].

作者信息

Auguściak-Duma Aleksandra, Sieroń Aleksander L

机构信息

Katedra i Zakład Biologii Molekularnej i Genetyki, Slaski Uniwersytet Medyczny.

出版信息

Postepy Hig Med Dosw (Online). 2008 Jan 14;62:148-65.

Abstract

Leiomyoma is a monoclonal benign tumor. It is often located in the muscle layer of the uterus in women of reproductive age. Its growth is accelerated by pregnancy and hormonal therapy. Its growth also depends on the concentration of sex hormones. Growth factors and cytokines may also participate in the formation of leiomyomas. The modulation of mitotic activity and abnormal extracellular matrix production are key elements of tumor growth. Elements of the TGFbeta superfamily are crucial factors in the proliferation of neoplasmic cells. TGF-beta1 and -beta3 stimulate the synthesis of various components of the extracellular matrix, but they also down-regulate the synthesis of proteinases which degrade the matrix, often leading to excessive overdeposition of connective tissue. Collagen types 1 and 3 are the main structural components of the extracellular matrix. The biosynthesis of collagens requires, among others, the action of procollagen C-endopeptidase, a protein of the BMP-1/mTLD subfamily. BMP-1/mTLD-like proteinases remove the carboxyl propeptides of procollagens 1, 2, and 3. Removal of the C-propeptides decreases the solubility of procollagens about 1000-fold to a concentration critical for their spontaneous self-assembly to collagen fibrils. Different substrates of BMP-1/mTLD are prolysyl oxidase, gamma2 chain of prolaminin, procollagen type VII, miostatin, dentin matrix protein 1, and perlekan. Due to the activation of various substrates by BMP-1/mTLDs, they are important regulators of the production of the extracellular matrix and its quality as well as of antiangiogenic responses by producing a factor from the basal membrane compound called perlekan. The BMP-1/mTLDs influence the formation of dorsal ventral patterning in embryos by releasing BMP-2/4 from the inhibitory protein chordin. Another aspect is induction of the development of muscle and neural tissue by activation of GDF8 and GDF11 as well as the regulation of growth and cell proliferation by releasing TGF-beta1 and -beta3 from latent complexes. Another yet poorly understood aspect is the evolution of neoplastic cells based on other than molecular genetic mechanisms. The detectable karyotype anomalies in tumor cells constitute just 40%. Therefore in this review the possible roles of extracellular matrix compounds and regulatory factors in the pathology of leiomyoma are discussed.

摘要

平滑肌瘤是一种单克隆良性肿瘤。它常位于育龄女性的子宫肌层。妊娠和激素治疗会加速其生长。其生长还取决于性激素的浓度。生长因子和细胞因子也可能参与平滑肌瘤的形成。有丝分裂活性的调节和异常的细胞外基质产生是肿瘤生长的关键因素。转化生长因子β(TGFβ)超家族的成员是肿瘤细胞增殖的关键因子。TGF-β1和-β3刺激细胞外基质各种成分的合成,但它们也下调降解基质的蛋白酶的合成,常常导致结缔组织过度沉积。1型和3型胶原蛋白是细胞外基质的主要结构成分。胶原蛋白的生物合成尤其需要原胶原C端肽酶的作用,它是BMP-1/mTLD亚家族的一种蛋白质。BMP-1/mTLD样蛋白酶去除原胶原1、2和3的羧基前肽。去除C前肽会使原胶原的溶解度降低约1000倍,达到其自发自组装成胶原纤维的临界浓度。BMP-1/mTLD的不同底物有脯氨酰氧化酶、层粘连蛋白γ2链、7型原胶原、肌肉生长抑制素、牙本质基质蛋白1和基底膜聚糖。由于BMP-1/mTLD对各种底物的激活作用,它们是细胞外基质产生及其质量以及通过从基底膜化合物基底膜聚糖产生一种因子而产生的抗血管生成反应的重要调节因子。BMP-1/mTLD通过从抑制蛋白腱蛋白中释放BMP-2/4来影响胚胎背腹模式的形成。另一个方面是通过激活生长分化因子8(GDF8)和生长分化因子11(GDF11)诱导肌肉和神经组织的发育,以及通过从潜伏复合物中释放TGF-β1和-β3来调节生长和细胞增殖。另一个尚未得到充分理解的方面是基于分子遗传机制以外的肿瘤细胞进化。肿瘤细胞中可检测到的核型异常仅占40%。因此,在本综述中讨论了细胞外基质化合物和调节因子在平滑肌瘤病理学中的可能作用。

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