Institute of Genetic Medicine and Howard Hughes Medical Institute, Johns Hopkins University School of Medicine, Baltimore, Maryland 21205, USA.
J Clin Invest. 2010 Feb;120(2):403-7. doi: 10.1172/JCI42014. Epub 2010 Jan 25.
TGF-beta regulates many aspects of cellular performance relevant to tissue morphogenesis and homeostasis. Postnatal perturbation of TGF-beta signaling contributes to the pathogenesis of many disease states, as recently exemplified through the study of Marfan syndrome (MFS), including aortic aneurysm and skeletal muscle myopathy. Heterogeneity in the regulation and consequences of TGF-beta signaling, amplified in the context of disease, has engendered confusion and controversy regarding its utility as a therapeutic target. Three studies recently published in the JCI, including one in this issue, underscore the complexity of this subject. Heydemann and colleagues implicate dimorphic variation in latent TGF-beta-binding protein 4 (LTBP4), a regulator of TGF-beta bioavailability and activation, as a modifier of muscular dystrophy in gamma-sarcoglycan-deficient mice. In contrast to experience with ascending aortic aneurysm in MFS, Wang and colleagues show that systemic abrogation of TGF-beta signaling worsens (rather than attenuates) Ang II-induced abdominal aortic aneurysm progression in mice. Tieu and colleagues define alterations in the regulation of vascular inflammation in the pathogenesis of Ang II-induced aneurysm and dissection in mice, which may help shed some light on this apparent paradox.
TGF-β 调节与组织形态发生和稳态相关的细胞功能的许多方面。TGF-β 信号的产后干扰导致许多疾病状态的发病机制,最近通过马凡综合征(MFS)的研究得到了例证,包括主动脉瘤和骨骼肌肌病。在疾病背景下,TGF-β 信号的调节和后果的异质性被放大,导致其作为治疗靶点的实用性存在混淆和争议。最近在《临床检查杂志》上发表的三项研究,包括本期的一项研究,强调了这一主题的复杂性。Heydemann 及其同事将潜在 TGF-β 结合蛋白 4(LTBP4)的二态性变异牵连进来,LTBP4 是 TGF-β 生物利用度和激活的调节剂,是 γ-横纹肌聚糖缺陷型小鼠肌肉营养不良的修饰因子。与 MFS 中的升主动脉瘤经验相反,Wang 及其同事表明,系统消除 TGF-β 信号会加重(而不是减弱)Ang II 诱导的小鼠腹主动脉瘤进展。Tieu 及其同事定义了血管炎症在 Ang II 诱导的小鼠动脉瘤和夹层发病机制中的调节变化,这可能有助于阐明这一明显的悖论。
