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体外增生性G细胞反应性

Hyperplastic G cell responsiveness in vitro.

作者信息

Gower W R, McSweeney E M, Fabri P J

出版信息

Surgery. 1985 Dec;98(6):1045-53.

PMID:3906974
Abstract

To evaluate the responsiveness of isolated, hyperplastic antral gastrin-producing G cells to a variety of secretagogues, hyperplastic hypergastrinemia was produced in Sprague-Dawley rats by fundusectomy. Mean serum immunoreactive gastrin (IRG) concentration was elevated fivefold above controls 4 days after operation and rose steadily to an eightfold increase at 66 days. Mean antral G cell density remained at control levels for as long as 7 days, increased twofold at 14 days, then remained between twofold and threefold greater than controls for as long as 66 days after operation. Antral mucosa IRG content increased from 141 +/- 38 (control) to 262 +/- 58 ng IRG/gm mucosa (4 to 6 weeks after fundusectomy). Crude fractions of dispersed antral mucosa cells enriched in G cells from fundusectomized rats contained 6.5% +/- 1.4% G cells with 0.19 +/- 0.6 pg IRG/G cell. Corresponding preparations from nonoperated rats contained 5.1% +/- 0.5% G cells with 0.07 +/- 0.02 pg IRG/G cell. Viability averaged greater than 95% for all preparations. Gastrin secretion was monitored in cell preparations further enriched in G cells (9% to 10%) by Percoll density gradient centrifugation either in the absence (basal) or presence of bombesin (1 mumol, 1 nmol/L), carbachol (1 mmol/L), leucine (10 mmol/L), and ethylamine (10 mmol/L). The basal secretory rate of hyperplastic G cell populations averaged 250% greater than normal G cell basal rates. Hyperplastic G cell preparations had an increased IRG secretory rate in the presence of bombesin (1 mumol/L, 750%; 1 nmol/L, 191%), leucine (120%), ethylamine (236%), and carbachol (183%). These conditions failed to increase the IRG secretory rate above basal in preparations from normal antra. Viable, dispersed, hyperplastic G cells have increased IRG content and basal IRG secretory rate and are functionally responsive to a variety of secretagogues.

摘要

为评估分离的、增生的胃窦产胃泌素G细胞对多种促分泌素的反应性,通过胃底切除术在Sprague-Dawley大鼠中诱导产生增生性高胃泌素血症。术后4天,血清免疫反应性胃泌素(IRG)平均浓度比对照组升高了五倍,并在66天时稳步上升至升高八倍。胃窦G细胞平均密度在长达7天的时间内保持在对照水平,在14天时增加了两倍,然后在术后长达66天的时间内保持比对照组高两倍至三倍。胃窦黏膜IRG含量从141±38(对照)增加到262±58 ng IRG/g黏膜(胃底切除术后4至6周)。来自胃底切除大鼠的富含G细胞的分散胃窦黏膜细胞粗提物含有6.5%±1.4%的G细胞,每个G细胞含0.19±0.6 pg IRG。来自未手术大鼠的相应制剂含有5.1%±0.5%的G细胞,每个G细胞含0.07±0.02 pg IRG。所有制剂的活力平均大于95%。通过Percoll密度梯度离心进一步富集G细胞(9%至10%)的细胞制剂中,在不存在(基础)或存在蛙皮素(1 μmol,1 nmol/L)、卡巴胆碱(1 mmol/L)、亮氨酸(10 mmol/L)和乙胺(10 mmol/L)的情况下监测胃泌素分泌。增生性G细胞群体的基础分泌率平均比正常G细胞基础分泌率高250%。在存在蛙皮素(1 μmol/L,750%;1 nmol/L,191%)、亮氨酸(120%)、乙胺(236%)和卡巴胆碱(183%)的情况下,增生性G细胞制剂的IRG分泌率增加。在正常胃窦的制剂中,这些条件未能使IRG分泌率高于基础水平。有活力的、分散的、增生性G细胞具有增加的IRG含量和基础IRG分泌率,并且对多种促分泌素具有功能反应性。

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