EXCESS IRON INTO HEPATOCYTES IS REQUIRED FOR ACTIVATION OF COLLAGEN TYPE-I GENE DURING EXPERIMENTAL SIDEROSIS

被引：61

作者：

GUALDI, R ^{[1
]}

CASALGRANDI, G ^{[1
]}

MONTOSI, G ^{[1
]}

VENTURA, E ^{[1
]}

PIETRANGELO, A ^{[1
]}

机构：

[1] UNIV MODENA,POLICLIN MODENA,DEPT INTERNAL MED,I-41100 MODENA,ITALY

来源：

GASTROENTEROLOGY | 1994年 / 107卷 / 04期

关键词：

D O I：

10.1016/0016-5085(94)90237-2

中图分类号：

R57 [消化系及腹部疾病];

学科分类号：

摘要：

Background/Aims: Liver fibrosis and cirrhosis represent common pathological findings in humans with iron overload. This study was undertaken to assess whether in vivo targeting of iron to liver parenchymal or nonparenchymal cells would differently affect collagen gene activity. Methods: Rats were treated with an iron diet or intramuscular injections of iron dextran, and in situ hybridization analyses on liver samples were performed. Results: These iron treatments determined parenchymal or reticuloendothelial cell iron overload, respectively. The typical distribution of iron into different liver cells was documented by histochemistry and confirmed by in situ hybridization analysis with a ferritin L complementary RNA probe. In iron-fed rats, in situ hybridization analysis identified a signal for collagen type I messenger RNA into nonparenchymal cells in zones I and ii. In rats with nonparenchymal cell iron overload, no activation of collagen gene expression was detected into or near iron-laden nonparenchymal cells. These findings were also confirmed by quantitative Northern blot analysis. Conclusions: The results of this study indicate that, regardless of the total hepatic iron burden, selective localization of iron into liver cells (i.e., parenchymal cells) is required for the activation of collagen gene during long-term iron overload in rodents.

引用

页码：1118 / 1124

页数：7

共 50 条

[21] TYPE-I COLLAGEN GENE-EXPRESSION IN DENTAL FOLLICLE CELLS
KASHNER, JE
KEYSER, JD
HEBERT, CA
NORRIS, K
SHROFF, B
JOURNAL OF DENTAL RESEARCH, 1995, 74 : 64 - 64
[22] STUDIES ON THE EXPRESSION OF TYPE-I COLLAGEN GENE IN A FINNISH MARFAN FAMILY
PULKKINEN, L
LEISTI, L
PALOTIE, A
AHO, S
PELTONEN, L
CYTOGENETICS AND CELL GENETICS, 1987, 46 (1-4): : 677 - 677
[23] TYPE-I COLLAGEN GENE-REGULATION AND THE MOLECULAR PATHOGENESIS OF CIRRHOSIS
BRENNER, DA
WESTWICK, J
BREINDL, M
AMERICAN JOURNAL OF PHYSIOLOGY, 1993, 264 (04): : G589 - G595
[24] ASSIGNMENT OF A STRUCTURAL GENE FOR TYPE-I COLLAGEN TO CHROMOSOME-7
SOLOMON, E
SYKES, B
CYTOGENETICS AND CELL GENETICS, 1978, 22 (1-6): : 281 - 284
[25] TRANSCRIPTIONAL ACTIVATION OF THE MOUSE MX GENE BY TYPE-I INTERFERON
STAEHELI, P
DANIELSON, P
HALLER, O
SUTCLIFFE, JG
MOLECULAR AND CELLULAR BIOLOGY, 1986, 6 (12) : 4770 - 4774
[26] QUANTITATIVE CHANGES IN INSOLUBLE COLLAGEN DURING ONTOGENY IN RODENTS (COLLAGEN TYPE-I AND TYPE-III)
DEYL, Z
ADAM, M
MECHANISMS OF AGEING AND DEVELOPMENT, 1977, 6 (01) : 25 - 33
[27] TYPE-I AND TYPE-VI COLLAGEN GENE-EXPRESSION IN KELOID TISSUE
SOLLBERG, S
PELTONEN, J
HSIAO, LL
JAAKKOLA, S
CHU, ML
UITTO, J
CLINICAL RESEARCH, 1990, 38 (02): : A656 - A656
[28] TYPE-I AND TYPE-VI COLLAGEN GENE-EXPRESSION IN KELOID TISSUE
SOLLBERG, S
PELTONEN, J
HSIAO, LL
JAAKKOLA, S
CHU, MI
UITTO, J
JOURNAL OF INVESTIGATIVE DERMATOLOGY, 1990, 94 (04) : 579 - 579
[29] ADHESION OF MOUSE HEPATOCYTES TO TYPE-I COLLAGEN - ROLE OF SUPRAMOLECULAR FORMS AND EFFECT OF PROTEOLYTIC DEGRADATION
BERMAN, A
MOROZEVICH, G
KARMANSKY, I
GLEIBERMAN, A
BYCHKOVA, V
BIOCHEMICAL AND BIOPHYSICAL RESEARCH COMMUNICATIONS, 1993, 194 (01) : 351 - 357
[30] ACTIVATION OF HUMAN NEUTROPHILS BY TYPE-I COLLAGEN - REQUIREMENT OF 2 DIFFERENT SEQUENCES
MONBOISSE, JC
BELLON, G
RANDOUX, A
DUFER, J
BOREL, JP
BIOCHEMICAL JOURNAL, 1990, 270 (02) : 459 - 462

← 1 2 3 4 5 →