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大鼠髓质内集合管中前列腺素E2的合成:对血管加压素依赖性环磷酸腺苷形成的影响。

Prostaglandin E2 synthesis in the inner medullary collecting duct of the rat: implications for vasopressin-dependent cyclic AMP formation.

作者信息

Jackson B A

出版信息

J Cell Physiol. 1986 Oct;129(1):60-4. doi: 10.1002/jcp.1041290109.

Abstract

The effects of osmolality on prostaglandin E2 (PGE2) biosynthetic capacity and the interaction between endogenous PGE2 synthesis and vasopressin (AVP)-dependent cyclic AMP generation were examined in papillary collecting ducts (PCD) microdissected from collagenase-digested rat kidneys. Increasing medium osmolality with NaCl:urea (1:2 molar ratio) progressively increased PGE2 synthesis in PCD up to 1,500 mOsm. Addition of NaCl:urea or NaCl alone were equally effective in stimulating PGE2 biosynthetic capacity in PCD. In contrast, addition of urea alone had a much smaller stimulatory effect on PGE2 synthesis. Inhibition of endogenous PGE2 synthesis with naproxen (10(-5)M) suppressed AVP-dependent cAMP formation in PCD when incubated in 300 mOsm medium but had no effect when incubated in 1,500 mOsm medium. Addition of 2.5 X 10(-5) M PGE2 also suppressed AVP-dependent cAMP formation in PCD only when incubated in 300 mOsm medium. The present study suggests that the PCD is a site of active PGE2 synthesis that is modulated by osmolality. Our results do not support the concept that endogenous PGE2 antagonizes vasopressin action via inhibition of AVP-dependent cAMP formation.

摘要

在从胶原酶消化的大鼠肾脏中显微分离出的肾乳头集合管(PCD)中,研究了渗透压对前列腺素E2(PGE2)生物合成能力的影响,以及内源性PGE2合成与血管加压素(AVP)依赖性环磷酸腺苷(cAMP)生成之间的相互作用。用氯化钠:尿素(摩尔比1:2)提高培养基渗透压,可使PCD中的PGE2合成逐渐增加,最高可达1500毫渗摩尔。添加氯化钠:尿素或单独添加氯化钠对刺激PCD中的PGE2生物合成能力同样有效。相比之下,单独添加尿素对PGE2合成的刺激作用要小得多。用萘普生(10^(-5)M)抑制内源性PGE2合成,在300毫渗摩尔培养基中孵育时可抑制PCD中AVP依赖性cAMP的形成,但在1500毫渗摩尔培养基中孵育时则无影响。仅在300毫渗摩尔培养基中孵育时,添加2.5×10^(-5)M PGE2也会抑制PCD中AVP依赖性cAMP的形成。本研究表明,PCD是活跃的PGE2合成位点,其受渗透压调节。我们的结果不支持内源性PGE2通过抑制AVP依赖性cAMP形成来拮抗血管加压素作用这一概念。

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