Kemal Ozbilgin M.Inan S.2024-07-222024-07-22200307703198http://akademikarsiv.cbu.edu.tr:4000/handle/123456789/20091Scleroderma is a connective tissue disorder characterised by excessive accumulation of collagen in the skin and internal organs. The most likely explanation for this process is local activation of collagen synthesis from fibroblasts. Our intention was to elucidate whether TGF-β3 and mast cells play a pathogenic role in abnormal connective tissue formation in scleroderma. In this study, skin biopsies from 20 patients with scleroderma and five from healthy individuals were studied by an indirect immunoperoxidase technique to determine the immunoreactivity of TGF-β3 in the dermis. In addition, skin samples were stained with toluidine blue to count the number of mast cells in scleroderma, and tissues were examined under the electron microscope to evaluate the ultrastructural changes. Increased TGF-β3 immunoreactivities were detected in the dermis in the patient's skin, suggesting the presence of a subpopulation responsible for the increased collagen production. Mast cell counts in the skin of patients with scleroderma were significantly greater (19.2 plusmn; 4.1/unit) than those of normal controls (4.4 ± 1.2/unit). Ultrastructural observations indicated that there is a close relationship between the mast cells and fibroblasts. These results suggest that fibrosis in scleroderma could evolve through the activation of fibroblasts and the regulatory mechanisms that appear to modulate the behavior of these cells with respect to collagen production.EnglishAdultBiological MarkersBiopsy, NeedleCase-Control StudiesCell MovementFemaleFibroblastsHumansImmunohistochemistryMaleMast CellsMicroscopy, ElectronMiddle AgedPhotomicrographyPrognosisReference ValuesScleroderma, LocalizedSensitivity and SpecificitySkinTransforming Growth Factor betaTransforming Growth Factor beta3collagentolonium chloridetransforming growth factor beta3adultarticlecell subpopulationcell ultrastructureclinical articlecollagen synthesiscontrolled studydermiselectron microscopefemalefibroblasthumanhuman tissueimmunohistochemistryimmunoperoxidase stainingimmunoreactivitymalemast cellpathogenesispriority journalregulatory mechanismsclerodermaskin biopsyskin fibrosisstatistical significancetransmission electron microscopyArticle10.1007/s10067-003-0706-5