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首页> 外文期刊>Pathology Research and Practice >Immunohistochemical study of type I collagen turn-over and of matrix metalloproteinases in chromoblastomycosis before and after treatment by terbinafine.
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Immunohistochemical study of type I collagen turn-over and of matrix metalloproteinases in chromoblastomycosis before and after treatment by terbinafine.

机译:特比萘芬治疗前后成色母细胞病中I型胶原蛋白转变和基质金属蛋白酶的免疫组织化学研究。

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摘要

The distribution of type I collagen, the major component of human dermis, was characterized by immunohistochemistry in skin lesions of chromoblastomycosis, a chronic cutaneous mycosis, before and after a specific antifungal treatment with terbinafine to study the changes induced in the lesions by the treatment. Newly synthesized type I collagen was studied with an antibody directed against the aminoterminal propeptide of the molecule (PINP), whereas mature, cross-linked type I collagen was detected with an antibody against the carboxyterminal telopeptide of type I collagen (ICTP). The isopeptide N epsilon gamma-glutamyl lysine (N epsilon gamma GL), synthesized by transglutaminase and able to cross-link several components of the extracellular matrix, has also been investigated with two monoclonal antibodies to determine if it is involved in the stabilisation of the fibrotic cutaneous lesions. The degradative process involved in the remodelling has also been assessed by immunohistochemistry with anti-metalloproteinase (MMP-1 and MMP-9) and anti-tissue inhibitor (TIMP-1) antibodies. All tissue macrophages stained for CD68 and MMP-9, but not for MMP-1, while the polymorphonuclear neutrophils had an elastase and a weak MMP-9 phenotype. The fibroblasts of fibrotic areas stained constantly for N epsilon gamma GL and PINP. The immunostaining of extracellular matrix for ICTP and N epsilon gamma GL, and the number of PINP-positive fibroblasts, decreased significantly after one year of antifungal treatment. Terbinafine treatment decreases the synthesis of type I collagen and leads to a partial reversal of the cutaneous fibrotic lesions, independently of the cure of the fungal infection.
机译:I型胶原蛋白(人真皮的主要成分)的分布通过在用特比萘芬进行特定的抗真菌治疗以研究治疗引起的病变变化之前和之后,在慢性皮肤真菌病的成色细胞霉菌病(慢性皮肤真菌病)的皮肤病变中进行了免疫组织化学表征。使用针对分子氨基末端前肽(PINP)的抗体研究了新合成的I型胶原蛋白,而使用针对I型胶原蛋白羧基端肽的抗体检测了成熟的交联I型胶原蛋白。还使用两种单克隆抗体研究了由转谷氨酰胺酶合成并能够交联细胞外基质几个成分的异肽N epsilonγ-谷氨酰赖氨酸(N epsilon gamma GL)。纤维化皮肤病变。还通过免疫组织化学使用抗金属蛋白酶(MMP-1和MMP-9)和抗组织抑制剂(TIMP-1)抗体对重塑中涉及的降解过程进行了评估。所有组织巨噬细胞均对CD68和MMP-9染色,但对MMP-1没有染色,而多形核中性粒细胞具有弹性蛋白酶和较弱的MMP-9表型。纤维化区域的成纤维细胞对NεγGL和PINP不断染色。经过一年的抗真菌治疗,ICTP和NεγGL的细胞外基质的免疫染色以及PINP阳性成纤维细胞的数量显着下降。特比萘芬治疗可减少I型胶原蛋白的合成,并导致皮肤纤维化病变的部分逆转,而与真菌感染的治愈无关。

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