HALOFUGINONE - AN INHIBITOR OF COLLAGEN TYPE-I SYNTHESIS

被引:108
作者
GRANOT, I
HALEVY, O
HURWITZ, S
PINES, M
机构
[1] AGR RES ORG,VOLCANI CTR,INST ANIM SCI,IL-50250 BET DAGAN,ISRAEL
[2] HEBREW UNIV JERUSALEM,FAC AGR,DEPT ANIM SCI,IL-76100 REHOVOT,ISRAEL
关键词
HALOFUGINONE; COLLAGEN; FIBROBLAST; CHONDROCYTE;
D O I
10.1016/0304-4165(93)90123-P
中图分类号
Q5 [生物化学]; Q7 [分子生物学];
学科分类号
071010 ; 081704 ;
摘要
The effect of halofuginone - a plant alkaloid used is a coccidiostat in birds - on collagen metabolism was studied various avian and mammalian cell cultures. In avian skin fibroblasts halofuginone attenuated the incorporation of [H-3]proline into collagenase-digestible proteins (CDP) at concentrations as low as 10(-11) M, without affecting production of [H-3]collagenase-non-digestible proteins (NCDP), cell proliferation or collagen degradation. Halofuginone depressed specifically the expression of alpha1 gene of collagen type I but not that of collagen type II. This was demonstrated in skin fibroblasts and growth-plate chondrocytes using probes containing inserts sequences corresponding to the alpha1(I) and alpha1(II) mRNAs. A slight inhibition of the expression of alpha2(I) was observed in avian skin fibroblasts but not in growth-plate chondrocytes. The inhibition of gene expression of both polypeptides of collagen type I in skin fibroblasts resulted in a decrease in synthesis, as demonstrated by immunoprecipitation with specific type I collagen antiserum. In primary cultures of mouse skin fibroblasts, avian epiphyseal growth plate chondrocytes and a rat embryo cell line - all of which produce and secrete collagen type I - halofuginone inhibited the incorporation of [H-3]proline into CDP, the Rat-I line being the most sensitive to the drug. These results suggest that halofuginone affects specifically type I collagen synthesis by repressing gene-expression. The need for extremely low concentrations of halofuginone to inhibit collagen type I synthesis, regardless of the tissue or animal species, contributes to the potential usefulness of the substance in studying collagen metabolism.
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页码:107 / 112
页数:6
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