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肝体阴而用阳理论在妇科临床运用中的探讨 被引量:3
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作者 谢秀超 彭卫东 刘晓玲 《四川中医》 2014年第4期52-53,共2页
"肝体阴而用阳"形象概括了肝体属阴而功能属阳的特点,此理论已广泛运用于临床各科,尤其是在中医妇科临床中,本文将针对肝体属阴而用阳的特性,阐述调肝体和调肝用的两种治法在妇科临床中的运用,目的是完善脏腑辨证在妇科辨证... "肝体阴而用阳"形象概括了肝体属阴而功能属阳的特点,此理论已广泛运用于临床各科,尤其是在中医妇科临床中,本文将针对肝体属阴而用阳的特性,阐述调肝体和调肝用的两种治法在妇科临床中的运用,目的是完善脏腑辨证在妇科辨证中的运用,和从肝论治妇科诸病的基础理论。 展开更多
关键词 妇科临床 调肝体 用治法方药
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The promoter analysis of the human C17orf25 gene, a novel chromosome 17pl3.3 gene 被引量:7
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作者 JIAN YING GUO, JIAN XU, DA QIN MAO, LI LI FU, JIAN REN GU, JING DE ZHUThe State-Key Laboratory of Oncogenes and Related Genes, Shanghai Cancer Institute, Ln 2200/25, Xie-Tu Road, Shanghai 200032, China 《Cell Research》 SCIE CAS CSCD 2002年第5期339-352,共14页
The human C17orf25 gene (Accession No. AF177342) is one of thirteen genes cloned from a region displaying a high score of loss of heterozygosity within chromosome 17pl3.3 in human hepatocellular carcinoma in China[l].... The human C17orf25 gene (Accession No. AF177342) is one of thirteen genes cloned from a region displaying a high score of loss of heterozygosity within chromosome 17pl3.3 in human hepatocellular carcinoma in China[l]. To unveil the underlying mechanisms for the transcription regulation of this gene and understand its implication to the hepatocellular carcinogenesis, we looked into the relevant aspects by both bioinformatic and experimental executions. We found: 1, The abundant expression of the C17orf25 gene was evident in all the cell lines and tissue samples tested, showing little hepatoma-selectivity; 2, Its transcription starts at a single site, locating at -60 from the translation initiation codon; 3, A 58 bp fragment containing the transcription start, extending from -112 to -55, represents the minimal promoter; 4, The consensus sequence within this fragment recognized by SP1 contributes predominantly to the activity of the minimal promoter; 5, The bioinformatic analysis suggests that the C17orf25 gene may encode a protein in the family of the glyoxalase. Our data has provided some deep insight into both function and regulation of the C1 7orf25 gene in the context of the normal liver and hepatocellular carcinoma. 展开更多
关键词 C17orf25 gene SP1 transcription regulation chromosome 17pl3.3.
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UP-REGULATION OF HEPATIC RECEPTOR FOR GROWTH HORMONE IN THE FLOUNDER ( PARALICHTHYS OLIVACEUS ) AFTER ORAL ADMINISTRATION WITH EXOGENOUS GH
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作者 刘宗柱 王金宝 +2 位作者 徐永立 王勇 张培军 《Chinese Journal of Oceanology and Limnology》 SCIE CAS CSCD 2001年第2期135-140,共6页
The iodination efficiency of salmon GH(sGH) was 38.82%,using a modification of the chloramine T method. The specific activity of the 125 I sGH was about 40 μCi/μg protein. The results of binding assay showed a singl... The iodination efficiency of salmon GH(sGH) was 38.82%,using a modification of the chloramine T method. The specific activity of the 125 I sGH was about 40 μCi/μg protein. The results of binding assay showed a single class of high affinity and low capacity binding site in flounder liver. Long term administration with exogenous GH can induce the up regulation of hepatic GH receptor in total binding capacity though there was no significant difference of association constant among any groups. Considering that there was no significant difference in capacity of free binding sites of livers from control and experimental fish, this result also indicated that the liver from experimental fish, compared to that from control fish, had more occupied binding sites. 展开更多
关键词 IODINATION GH hepatic receptor up regulation
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Bile-acid-activated farnesoid X receptor regulates hydrogen sulfide production and hepatic microcirculation 被引量:8
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作者 Barbara Renga Andrea Mencarelli +2 位作者 Marco Migliorati Eleonora Distrutti Stefano Fiorucci 《World Journal of Gastroenterology》 SCIE CAS CSCD 2009年第17期2097-2108,共12页
AIM: To investigate whether the farnesoid X receptor (FXR) regulates expression of liver cystathionase (CSE), a gene involved in hydrogen sulfi de (H2S) generation. METHODS: The regulation of CSE expression in respons... AIM: To investigate whether the farnesoid X receptor (FXR) regulates expression of liver cystathionase (CSE), a gene involved in hydrogen sulfi de (H2S) generation. METHODS: The regulation of CSE expression in response to FXR ligands was evaluated in HepG2 cells and in wild-type and FXR null mice treated with 6-ethyl chenodeoxycholic acid (6E-CDCA), a synthetic FXR ligand. The analysis demonstrated an FXR responsive element in the 5'-flanking region of the human CSE gene. The function of this site was investigated by luciferase reporter assays, chromatin immunoprecipitation and electrophoretic mobility shift assays. Livers obtained from rats treated with carbon tetrachloride alone, or in combination with 6-ethyl chenodeoxycholic acid, were studied for hydrogen sulphide generation and portal pressure measurement. RESULTS: Liver expression of CSE is regulated by bile acids by means of an FXR-mediated mechanism. Western blotting, qualitative and quantitative polymerase chain reaction, as well as immunohistochemical analysis, showed that expression of CSE in HepG2 cells and in mice is induced by treatment with an FXR ligand. Administration of 6E-CDCA to carbon tetrachloride treated rats protected against the down-regulation of CSE expression, increased H2S generation, reduced portal pressure and attenuated the endothelial dysfunction of isolated and perfused cirrhotic rat livers. CONCLUSION: These results demonstrate that CSE is an FXR-regulated gene and provide a new molecular explanation for the pathophysiology of portal hypertension. 展开更多
关键词 Nuclear receptor Farnesoid X receptor Cystathionase Hydrogen sulfide Portal hypertension
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