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结缔组织激活。十五。一种多形核白细胞因子对糖胺聚糖和DNA合成的刺激作用。

Connective tissue activation. XV. Stimulation of glycosaminoglycan and DNA synthesis by a polymorphonuclear leukocyte factor.

作者信息

Myers S L, Castor C W

出版信息

Arthritis Rheum. 1980 May;23(5):556-63. doi: 10.1002/art.1780230506.

Abstract

Human synovial fibroblasts in culture have been stimulated to augment hyaluronate synthesis and glucose utilization by connective tissue activating peptides (CTAP) extracted from human spleen, lymphocytes, platelets, granulocytes, and tumour cells. The platelet-derived mediator CTAP-III also stimulated DNA synthesis in synovial fibroblasts, but CTAP-I from lymphocytes and spleen did not. The present study demonstrates the mitogenic potential of a granulocyte mediator (CTAP-PMN). Normal granulocytes were prepared with Ficoll-diatrizoate gradients, platelet contamination being estimated by phase microscopy and by radioimmunoassay for the platelet-specific protein, beta-thromboglobulin. CTAP-PMN preparations derived from 4 x 10(7) cells/ml stimulated culture 3H-thymidine incorporation to 3.56 +/- 1.32 (SD) times control levels. Although exposure of preparations to thiols reduced their mitogenicity, CTAP-PMN was relatively heat-stable. SDS gel electrophoresis of active fractions suggested a molecular weight between 12,700 and 15,700 daltons. In double immunodiffusion, antisera to CTAP-III showed no reactivity with CTAP-PMN. CTAP-PMN or other granulocyte factors capable of stimulating fibroblast DNA synthesis may play a role in chronic proliferative synovitis or in other settings where exudative inflammation is accompanied by connective tissue growth.

摘要

培养的人滑膜成纤维细胞已被来自人脾脏、淋巴细胞、血小板、粒细胞和肿瘤细胞的结缔组织激活肽(CTAP)刺激,以增强透明质酸合成和葡萄糖利用。血小板衍生介质CTAP-III也刺激滑膜成纤维细胞中的DNA合成,但淋巴细胞和脾脏来源的CTAP-I则无此作用。本研究证明了粒细胞介质(CTAP-PMN)的促有丝分裂潜力。用Ficoll-泛影葡胺梯度制备正常粒细胞,通过相差显微镜和针对血小板特异性蛋白β-血小板球蛋白的放射免疫测定法估算血小板污染情况。源自4×10⁷个细胞/毫升的CTAP-PMN制剂将培养的³H-胸腺嘧啶核苷掺入量刺激至对照水平的3.56±1.32(标准差)倍。尽管将制剂暴露于硫醇会降低其促有丝分裂活性,但CTAP-PMN相对耐热。活性组分的SDS凝胶电泳表明分子量在12,700至15,700道尔顿之间。在双向免疫扩散中,抗CTAP-III血清与CTAP-PMN无反应性。CTAP-PMN或其他能够刺激成纤维细胞DNA合成的粒细胞因子可能在慢性增殖性滑膜炎或其他渗出性炎症伴有结缔组织生长的情况下发挥作用。

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