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Amine precursor uptake and decarboxylation: significance for processing of the rat gastrin precursor.

机译:胺前体的吸收和脱羧:对大鼠胃泌素前体的加工具有重要意义。

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1. Conversion of prohormone precursors to smaller active products occurs in secretory granules, which also have the capacity to concentrate biogenic amines. We have examined how processing of the gastrin precursor, progastrin, in rat antral mucosa is influenced by modulation of the biogenic amine content of secretory granules. 2. Newly synthesized progastrin-derived peptides in rat antral mucosa were labelled in vitro with 35SO4(2-) using a pulse-chase protocol and detected after immunoprecipitation by HPLC with on-line liquid scintillation counting. Secretory granule morphology was examined by electron microscopy. The effects of experimentally manipulating secretory granule pH and amine content were examined. 3. The dopamine precursor L-beta-3,4-dihydroxyphenylalanine (L-DOPA) inhibited cleavage of 35S-labelled thirty-four amino acid amidated gastrin, i.e. [35S]G34, and of [35S]G34 with COOH-terminal glycine, i.e. [35S]G34-Gly, at a pair of lysine residues, but did not influence cleavage of progastrinat pairs of arginine residues. The effect of L-DOPA was reversed by reserpine, which inhibits the amine-proton exchangers VMAT1 and VMAT2, and by carbidopa, which inhibits aromatic L-amino acid decarboxylase. 4. Treatments that raise intragranular pH, e.g. the weak base chloroquine, the ionophore monensin and the vacuolar proton pump inhibitor bafilomycin A1, had similar effects to L-DOPA. 5. Electron microscopical studies showed that the electron-dense aggregrates in gastrin cell secretory granules were lost after inhibition of the vacuolar proton pump. Treatment with L-DOPA produced reserpine-sensitive dissipation of the electron-dense aggregates, compatible with the idea that increased amine delivery raised intragranular pH. 6. The data suggest that the processes of amine precursor uptake, decarboxylation and sequestration in secretory granules are associated with selective modulation of progastrin cleavage, possibly by raising intragranular pH and thereby inhibiting pH-sensitive prohormone convertases.
机译:1.前激素原转化为较小的活性产物发生在分泌颗粒中,分泌颗粒也具有浓缩生物胺的能力。我们已经检查了大鼠胃窦粘膜中胃泌素前体前胃泌素的加工如何受到分泌颗粒生物胺含量的调节的影响。 2.使用脉冲追逐方案在体外用大鼠的胃窦黏膜中新合成的前胃泌素衍生肽标记35SO4(2-),并在HPLC免疫沉淀和在线液体闪烁计数后进行检测。通过电子显微镜检查分泌颗粒的形态。检查了通过实验操作分泌颗粒的pH和胺含量的效果。 3.多巴胺前体L-β-3,4-二羟基苯丙氨酸(L-DOPA)抑制35S标记的34个氨基酸酰胺化胃泌素,即[35S] G34和[35S] G34的COOH末端甘氨酸裂解。 ,即[35S] G34-Gly,位于一对赖氨酸残基上,但不影响精氨酸残基的前前列腺素对的裂解。利血平可抑制胺-质子交换剂VMAT1和VMAT2,卡比多巴可抑制芳族L-氨基酸脱羧酶,可逆转L-DOPA的作用。 4.提高颗粒内pH的处理,例如。弱碱氯喹,离子载体莫能菌素和液泡质子泵抑制剂bafilomycin A1与L-DOPA具有相似的作用。 5.电子显微镜研究表明,抑制液泡质子泵后,胃泌素细胞分泌颗粒中的电子致密聚集体丢失。用L-DOPA处理会产生利血平敏感的电子致密聚集体消散,这与增加胺释放量会提高颗粒内pH值的想法兼容。 6.数据表明,分泌颗粒中胺前体的摄取,脱羧和螯合过程与前胃泌素裂解的选择性调节有关,可能是通过提高颗粒内pH值,从而抑制了对pH敏感的激素原转化酶。

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