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腹部照射后大鼠远端结肠中血管活性肠肽刺激的环磷酸腺苷途径的改变

Alterations of the VIP-stimulated cAMP pathway in rat distal colon after abdominal irradiation.

作者信息

Morel E, Dublineau I, Lebrun F, Griffiths N M

机构信息

Institut de Protection et de Sûreté Nucléaire, Département de Protection et de la santé de l'Homme et de Dosimétrie, Section Autonome de Radiobiologie Appliquée à la Médecine, F-92265 Fontenay-aux-Roses Cedex, France.

出版信息

Am J Physiol Gastrointest Liver Physiol. 2002 May;282(5):G835-43. doi: 10.1152/ajpgi.00457.2001.

Abstract

Ionizing radiation induces hyporesponsiveness of rat colonic mucosa to vasoactive intestinal peptide (VIP). Possible mechanisms responsible for this hyporesponsiveness of the cAMP communication pathway in rat colon were investigated. VIP- and forskolin-stimulated short-circuit current (I(sc)) responses were studied after a 10-Gy abdominal irradiation in Ussing chambers as well as in single, isolated crypts. Adenylyl cyclase (AC) activity and VIP receptor characteristics were determined in mucosal membrane preparations. In addition, alterations in crypt morphology were studied. Impaired secretory responses to VIP and forskolin were observed 4 days after irradiation (decrease of 80%). cAMP analog-stimulated I(sc) responses were unchanged. In isolated crypts, VIP- and forskolin-stimulated cAMP accumulation was markedly reduced by 80 and 50%, respectively. VIP-stimulated AC activity and VIP receptor number were decreased in membrane preparations. No major change of cellularity was associated with these functional alterations. In conclusion, the decreased secretory responses to VIP of rat colon are associated with reduced cAMP accumulation, decreased AC activity, and diminution of VIP receptor numbers without a marked decrease of crypt cell number.

摘要

电离辐射可诱导大鼠结肠黏膜对血管活性肠肽(VIP)反应性降低。本研究探讨了大鼠结肠中cAMP信号通路反应性降低的可能机制。采用Ussing室及单个分离隐窝,研究了10 Gy腹部照射后VIP和福斯高林刺激的短路电流(I(sc))反应。测定了黏膜膜制剂中的腺苷酸环化酶(AC)活性和VIP受体特性。此外,还研究了隐窝形态的变化。照射后4天观察到对VIP和福斯高林的分泌反应受损(降低80%)。cAMP类似物刺激的I(sc)反应未改变。在分离的隐窝中,VIP和福斯高林刺激的cAMP积累分别显著降低了80%和50%。膜制剂中VIP刺激的AC活性和VIP受体数量减少。这些功能改变未伴有细胞数量的明显变化。总之,大鼠结肠对VIP的分泌反应降低与cAMP积累减少、AC活性降低和VIP受体数量减少有关,而隐窝细胞数量无明显减少。

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