We produced transgenic mice that express a dominant-positive truncated form of sterol regulatory element-binding protein-2 (SREBP-2) in liver and adipose tissue. The encoded protein lacks the membrane-binding and COOH-terminal regulatory domains, and it is therefore not susceptible to negative regulation by cholesterol. Livers from the transgenic mice showed increases in mRNAs encoding multiple enzymes of cholesterol biosynthesis, the LDL receptor, and fatty acid biosynthesis. The elevations in mRNA for 3-hydroxy-3-methylglutaryl coenzyme A (HMG CoA) synthase and HMG CoA reductase were especially marked (13-fold and 75-fold, respectively). As a result, the transgenic livers showed a 28-fold increase in the rate of cholesterol synthesis and a lesser fourfold increase in fatty acid synthesis, as measured by intraperitoneal injection of [3H]water. These results contrast with previously reported effects of dominant-positive SREBP-1a, which activated fatty acid synthesis more than cholesterol synthesis. In adipose tissue of the SREBP-2 transgenics, the mRNAs for cholesterol biosynthetic enzymes were elevated, but the mRNAs for fatty acid biosynthetic enzymes were not. We conclude that SREBP-2 is a relatively selective activator of cholesterol synthesis, as opposed to fatty acid synthesis, in liver and adipose tissue of mice.
J D Horton, I Shimomura, M S Brown, R E Hammer, J L Goldstein, H Shimano
Title and authors | Publication | Year |
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Palmitic acid induces central leptin resistance and impairs hepatic glucose and lipid metabolism in male mice
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The Journal of Nutritional Biochemistry | 2015 |
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Metabolite profiling in plasma and tissues of ob/ob and db/db mice identifies novel markers of obesity and type 2 diabetes
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Diabetologia | 2015 |
Chronological analysis of caloric restriction-induced alteration of fatty acid biosynthesis in white adipose tissue of rats
N Okita, T Tsuchiya, M Fukushima, K Itakura, K Yuguchi, T Narita, Y Hashizume, Y Sudo, T Chiba, I Shimokawa, Y Higami |
Experimental Gerontology | 2015 |
AICAR-Induced Activation of AMPK Inhibits TSH/SREBP-2/HMGCR Pathway in Liver
S Liu, F Jing, C Yu, L Gao, Y Qin, J Zhao, M Zang |
PloS one | 2015 |
Response of the Cholesterol Metabolism to a Negative Energy Balance in Dairy Cows Depends on the Lactational Stage
JJ Gross, EC Kessler, C Albrecht, RM Bruckmaier |
PloS one | 2015 |
Regulation of SREBPs by Sphingomyelin in Adipocytes via a Caveolin and Ras-ERK-MAPK-CREB Signaling Pathway
N Makdissy, K Haddad, C Mouawad, I Popa, M Younsi, P Valet, L Brunaud, O Ziegler, D Quilliot, D Delmas |
PloS one | 2015 |
IAVPGEVA, IAVPTGVA, and LPYP, three peptides from soy glycinin, modulate cholesterol metabolism in HepG2 cells through the activation of the LDLR-SREBP2 pathway
C Lammi, C Zanoni, A Arnoldi |
Journal of Functional Foods | 2015 |
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CL Pinto, SM Kalasekar, CW McCollum, A Riu, P Jonsson, J Lopez, EC Swindell, A Bouhlatouf, P Balaguer, M Bondesson, JÅ Gustafsson |
Molecular and Cellular Endocrinology | 2015 |
Hepatic S1P deficiency lowers plasma cholesterol levels in apoB-containing lipoproteins when LDLR function is compromised
D Basu, A Huq, J Iqbal, MM Hussain, XC Jiang, W Jin |
Nutrition & Metabolism | 2015 |
Identification of human ELOVL5 enhancer regions controlled by SREBP
A Shikama, H Shinozaki, Y Takeuchi, T Matsuzaka, Y Aita, T Murayama, Y Sawada, X Piao, N Toya, Y Oya, A Takarada, Y Masuda, M Nishi, M Kubota, Y Izumida, Y Nakagawa, H Iwasaki, K Kobayashi, S Yatoh, H Suzuki, H Yagyu, Y Kawakami, N Yamada, H Shimano, N Yahagi |
Biochemical and Biophysical Research Communications | 2015 |
Fatostatin, an SREBP inhibitor, prevented RANKL-induced bone loss by suppression of osteoclast differentiation
K Inoue, Y Imai |
Biochimica et Biophysica Acta (BBA) - Molecular Basis of Disease | 2015 |
The effects of vitamin D3 on lipogenesis in the liver and adipose tissue of pregnant rats
EJ Kang, JE Lee, SM An, J Lee, H Kwon, B Kim, S Kim, J Kim, D Hwang, YJ Jung, S Yang, S Kim, BS An |
International journal of molecular medicine | 2015 |
Sirtuins in glucose and lipid metabolism
X Ye, M Li, T Hou, T Gao, W Zhu, Y Yang |
Oncotarget | 2015 |