CONDITIONALLY IMMORTALIZED HEPATOCYTES FROM LONG-EVANS CINNAMON (LEC) RATS - AN IN-VITRO MODEL FOR GENE REPLACEMENT THERAPY FOR WILSONS-DISEASE

被引：0

作者：

SCHILSKY, ML ^{[1
]}

KABISCHER, S ^{[1
]}

MANCHIKALAPUDI, P ^{[1
]}

PRIMUS, LH ^{[1
]}

机构：

[1] ALBERT EINSTEIN COLL MED,MARION BESSIN LIVER RES CTR,BRONX,NY 10467

来源：

HEPATOLOGY | 1995年 / 22卷 / 04期

关键词：

D O I：

暂无

中图分类号：

R57 [消化系及腹部疾病];

学科分类号：

摘要：

引用

页码：1065 / 1065

页数：1

共 32 条

[21] Role of p38 Mapk in Development of Acute Hepatic Injury in Long-Evans Cinnamon (LEC) Rats, an Animal Model of Human Wilson's Disease
Kadowaki, Shingo
Meguro, Saori
Imaizumi, Yoshitaka
Sakai, Hiroshi
Endoh, Daiji
Hayashi, Masanobu
JOURNAL OF VETERINARY MEDICAL SCIENCE, 2013, 75 (12): : 1551 - 1556
[22] Mechanism of hepatorenal syndrome in rats of Long-Evans Cinnamon strain, an animal model of fulminant Wilson's disease
Nomiyama, K
Nomiyama, H
Kameda, N
Tsuji, A
Sakurai, H
TOXICOLOGY, 1999, 132 (2-3) : 201 - 214
[23] REMOVAL OF COPPER FROM THE LIVER OF LONG-EVANS CINNAMON (LEC) RATS BY TETRATHIOMOLYBDATE (TTM) INJECTION - THE MAIN EXCRETION ROUTE IS VIA BLOOD, NOT BILE
SUGAWARA, N
LI, D
SUGAWARA, C
RESEARCH COMMUNICATIONS IN MOLECULAR PATHOLOGY AND PHARMACOLOGY, 1994, 85 (02) : 217 - 226
[24] Ferrous and ferric iron accumulates in the brain of aged Long-Evans Cinnamon rats, an animal model of Wilson's disease
Kim, JM
Ko, SB
Kwon, SJ
Kim, HJ
Han, MK
Kim, DW
Cho, SS
Jeon, BS
NEUROSCIENCE LETTERS, 2005, 382 (1-2) : 143 - 147
[25] COPPER-METABOLISM AT 2 STAGES IN THE ONSET OF SPONTANEOUS HEPATITIS IN NEW MUTANT LONG-EVANS CINNAMON (LEC) RATS - INDUCTION OF HEPATIC COPPER-METALLOTHIONEIN AND ITS LEAKAGE FROM HEPATOCYTES
SUGAWARA, N
SUGAWARA, C
SATO, M
MORI, M
JOURNAL OF TRACE ELEMENTS IN EXPERIMENTAL MEDICINE, 1993, 6 (01): : 15 - 21
[26] Increased abundance of GABA, receptor subunit mRNAs in the brain of Long-Evans Cinnamon rats, an animal model of Wilson's disease
Follesa, P
Mallei, A
Floris, S
Mostallino, MC
Sanna, E
Biggio, G
MOLECULAR BRAIN RESEARCH, 1999, 63 (02): : 268 - 275
[27] BILIARY-EXCRETION OF COPPER, METALLOTHIONEIN, AND GLUTATHIONE INTO LONG-EVANS CINNAMON RATS - A CONVINCING ANIMAL-MODEL FOR WILSON DISEASE
SUGAWARA, N
SATO, M
YUASA, M
SUGAWARA, C
BIOCHEMICAL AND MOLECULAR MEDICINE, 1995, 55 (01) : 38 - 42
[28] Dietary polyunsaturated fatty acids suppress acute hepatitis, alter gene expression and prolong survival of female Long-Evans Cinnamon rats, a model of Wilson disease
Du, CY
Fujii, Y
Ito, M
Harada, M
Moriyama, E
Shimada, R
Ikemoto, A
Okuyama, H
JOURNAL OF NUTRITIONAL BIOCHEMISTRY, 2004, 15 (05): : 273 - 280
[29] Protection from spontaneous hepatocellular damage by N-benzyl-D-glucamine dithiocarbamate in Long-Evans Cinnamon rats, an animal model of Wilson's disease
Shimada, H
Takahashi, M
Shimada, A
Okawara, T
Yasutake, A
Imamura, Y
Kiyozumi, M
TOXICOLOGY AND APPLIED PHARMACOLOGY, 2005, 202 (01) : 59 - 67
[30] Comparison of urinary excretion of phenolsulfonphthalein in an animal model for Wilson's disease (Long-Evans Cinnamon rats) with that in normal Wistar rats: Involvement of primary active organic anion transporter.
Itagaki, S
Shimamoto, S
Hirano, T
Iseki, K
JOURNAL OF PHARMACY AND PHARMACEUTICAL SCIENCES, 2004, 7 (02): : 227 - 234

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