CHARACTERIZATION OF NUCLEAR ANGIOTENSIN-II-BINDING SITES IN RAT-LIVER AND COMPARISON WITH PLASMA-MEMBRANE RECEPTORS

被引:91
作者
TANG, SS [1 ]
ROGG, H [1 ]
SCHUMACHER, R [1 ]
DZAU, VJ [1 ]
机构
[1] HARVARD UNIV, BRIGHAM & WOMENS HOSP, SCH MED, DIV VASC MED & ATHEROSCLEROSIS, BOSTON, MA 02115 USA
关键词
D O I
10.1210/en.131.1.374
中图分类号
R5 [内科学];
学科分类号
1002 ; 100201 ;
摘要
Although the action of angiotensin-II (Ang-II) is believed to be mediated by a transmembrane signal transduction mechanism, accumulating evidence suggests that Ang-II may also have a direct nuclear action. We have characterized the nuclear Ang-II-binding site in purified nuclei preparation from rat liver and compared it to plasma membrane Ang-II receptors. [I-125]Ang-II binding to isolated nuclei reached equilibration in 30 min at 25 C, slower than binding to plasma membrane, which reached equilibration within 10 min. Scatchard analysis of [I-125]Ang-II binding to isolated nuclei revealed a single class of binding sites (K(d) = 1.4 nM; binding capacity = 10 fmol/mg protein or 460 sites/nucleus). In the nuclear preparation, Ang-II and its fragments competed for binding a potency order of Ang-III = Ang-II > Ang-II-(1-7) > Ang-II-(1-6) > Ang-II-(1-5). Losartan potassium (DuP 753), a selective blocker of the Ang-II receptor subtype I, fully inhibits nuclear Ang-11 binding with affinity similar to that in plasma membrane. The pH optimum for [I-125]Ang-II binding to nuclei was 7.0, while binding to plasma membrane was optimal at pH 8.0. Low concentrations (0.05-0.1 mM) of dithiothreitol increased [I-125]Ang-II binding to nuclei, but not to plasma membrane. In the absence of detergent, Ang-II-binding sites appear to consist of soluble protein releasable from nuclei by freezing and thawing, hence distinct in physicochemical properties from the membrane-bound receptor. Size-exclusion HPLC estimated the mol wt of the soluble Ang-II-binding sites to be 66 kilodaltons. These nuclear Ang-II-binding sites have some similarities to but also show notable physicochemical differences from plasma membrane Ang-II receptors, and they may play a role in mediating the intracellular action of Ang-II.
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页码:374 / 380
页数:7
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