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骨骼组织对细胞因子的反应。

Skeletal tissue response to cytokines.

作者信息

Goldring M B, Goldring S R

机构信息

Department of Medicine, Harvard Medical School, Boston.

出版信息

Clin Orthop Relat Res. 1990 Sep(258):245-78.

PMID:2203572
Abstract

Communication among individual cell types that populate connective tissues such as cartilage or bone is of critical importance in determining the phenotypic properties of these tissues under both physiologic and pathologic conditions. Cytokines, which may be defined as soluble products released from one cell that can modulate the activity of other cells, play a critical role in this process of cell communication. The introduction of molecular biologic techniques has permitted identification of specific cytokines previously characterized on the basis of biologic activities. Cloning and sequencing of these products have provided formal evidence for their existence and allowed identification of the full spectrum of their biologic activities. These results have established that individual cytokines may have multiple biologic activities and that multiple cytokines share common functional properties. Based on these results, the term "cytokine" has been used more generally to include products originally described as growth or differentiation factors, e.g., interleukins, monokines, or lymphokines. Cytokines have an important role in the initiation and control of skeletal tissue growth and development and in regulating bone remodeling in the adult organism. As in other connective tissues, these effects are mediated via paracrine, autocrine, and endocrine mechanisms. In skeletal tissues, cytokines may modulate the activity of resident cells by an additional mechanism. Factors produced locally within bone or arriving via the circulation are incorporated into the mineralized bone matrix, and their release during skeletal remodeling could provide the basis for coupling the activity of bone resorbing and forming cells. The principal cytokines that have been shown to affect skeletal tissues include factors previously described as monokines or lymphokines such as interleukin-1 (IL-1), tumor necrosis factors (TNF-alpha and TNF-beta), and interferon-gamma (IFN-gamma); the colony-stimulating factors; and the so-called growth and differentiation factors including transforming growth factors-alpha and -beta (TGF-alpha and TGF-beta), insulinlike growth factor-I (IGF-I), platelet-derived growth factor (PDGF), and fibroblast growth factor (FGF). Although the effects of the individual cytokines are diverse, it is possible to classify individual factors based on their effects on specific aspects of bone formation or resorption. Significant progress has been made recently toward elucidating the mechanisms of action of the cytokines. Binding studies using radiolabeled ligands have characterized the specific cell surface receptors and defined their distribution and properties among skeletal tissue cells. Various so-called signal transduction pathways have been implicated in mediating these effects...

摘要

构成软骨或骨等结缔组织的单个细胞类型之间的通讯,对于确定这些组织在生理和病理条件下的表型特性至关重要。细胞因子可定义为从一个细胞释放的能调节其他细胞活性的可溶性产物,在这一细胞通讯过程中起关键作用。分子生物学技术的引入使得能够鉴定出先前基于生物学活性而被描述的特定细胞因子。这些产物的克隆和测序为它们的存在提供了确切证据,并有助于确定其全部生物学活性范围。这些结果表明,单个细胞因子可能具有多种生物学活性,并且多种细胞因子具有共同的功能特性。基于这些结果,“细胞因子”一词已被更广泛地使用,以包括最初被描述为生长或分化因子的产物,例如白细胞介素、单核因子或淋巴因子。细胞因子在骨骼组织生长和发育的启动与控制以及调节成年生物体的骨重塑中起重要作用。与其他结缔组织一样,这些作用是通过旁分泌、自分泌和内分泌机制介导的。在骨骼组织中,细胞因子可能通过另一种机制调节驻留细胞的活性。在骨内局部产生或通过循环到达的因子会整合到矿化的骨基质中,它们在骨骼重塑过程中的释放可为骨吸收细胞和骨形成细胞活性的耦联提供基础。已证明对骨骼组织有影响的主要细胞因子包括先前被描述为单核因子或淋巴因子的因子,如白细胞介素 -1(IL -1)、肿瘤坏死因子(TNF -α和TNF -β)以及干扰素 -γ(IFN -γ);集落刺激因子;以及所谓的生长和分化因子,包括转化生长因子 -α和 -β(TGF -α和TGF -β)、胰岛素样生长因子 -I(IGF -I)、血小板衍生生长因子(PDGF)和成纤维细胞生长因子(FGF)。尽管单个细胞因子的作用多种多样,但根据它们对骨形成或吸收特定方面的影响对单个因子进行分类是可能的。最近在阐明细胞因子的作用机制方面取得了重大进展。使用放射性标记配体的结合研究已确定了特定的细胞表面受体,并明确了它们在骨骼组织细胞中的分布和特性。各种所谓的信号转导途径已被认为参与介导这些作用……

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