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牛阴茎退缩肌提取物中平滑肌抑制因子的一些理化性质。

Some physical and chemical properties of the smooth muscle inhibitory factor in extracts of the bovine retractor penis muscle.

作者信息

Gillespie J S, Hunter J C, Martin W

出版信息

J Physiol. 1981 Jun;315:111-25. doi: 10.1113/jphysiol.1981.sp013736.

Abstract
  1. A method of extracting and partially purifying a smooth muscle inhibitory factor from the bovine retractor penis is described. This consists of extraction in methanol followed by adsorption on an anion exchange resin, elution from the resin with 500 mM-sodium chloride solution and, if necessary, removal of adenine nucleotides by adsorption on alumina. 2. The inhibitory factor exists in a stable pharmacologically inactive form and an unstable pharmacologically active form. Conversion to the active form is by a brief exposure to acid at pH 2.0. 3. The inhibitory factor is insoluble in ether or acetone but soluble in methanol. Anhydrous methanol, however, irreversibly destroys pharmacological activity especially if the inhibitory factor is in the active form. This effect of methanol is prevented by the presence of 20-30-% water. 4. The inhibitory factor binds to an anion exchange resin but not to a cation exchange resin. It can be eluted from the resin by 500 mM-sodium chloride solution. 5. The molecular weight of the inhibitory factor, as judged by the ability to pass ultrafiltration membranes, is about 500. 6. Inhibitory activity is unaffected by the proteases trypsin, subtilisin or pepsin or by leucine aminopeptidase, pyroglutamate aminopeptidase or carboxypeptidase. The inhibitory effect of the extract and the inhibitory response to stimulation of the non-adrenergic, non-cholinergic nerves are also unaffected by the protease inhibitor, aprotinin. The active material, therefore, is unlikely to be a peptide. 7. Inhibitory activity is abolished by exposure of the extracts to periodic acid or sodium periodate. Acetic anhydride in pyridine also abolishes activity but the vehicle pyridine is also effective. 8. Sodium borohydride but not borate abolishes inhibitory activity when added to the acid-activated material at pH 2.0 but has no effect or may even potentiate activity if added to the stable inactive form at pH 9.0. When added to the acid-activated but neutralized material at pH 6.8 it usually abolishes inhibitory activity but occasionally has no effect. 9. These results suggest the smooth muscle inhibitory factor in these extracts is potent and probably novel. It does not appear to be a peptide or a lipid but may contain a carbohydrate as part of the molecule. Its possible physiological role is discussed.
摘要
  1. 本文描述了一种从牛阴茎退缩肌中提取并部分纯化平滑肌抑制因子的方法。该方法包括用甲醇提取,然后吸附于阴离子交换树脂上,用500 mM氯化钠溶液从树脂上洗脱,如有必要,通过吸附于氧化铝上去除腺嘌呤核苷酸。2. 抑制因子以稳定的药理无活性形式和不稳定的药理活性形式存在。通过在pH 2.0下短暂暴露于酸可转化为活性形式。3. 抑制因子不溶于乙醚或丙酮,但溶于甲醇。然而,无水甲醇会不可逆地破坏药理活性,尤其是当抑制因子处于活性形式时。甲醇的这种作用可通过存在20 - 30%的水来防止。4. 抑制因子与阴离子交换树脂结合,但不与阳离子交换树脂结合。它可以用500 mM氯化钠溶液从树脂上洗脱。5. 根据通过超滤膜的能力判断,抑制因子的分子量约为500。6. 抑制活性不受蛋白酶胰蛋白酶、枯草杆菌蛋白酶或胃蛋白酶或亮氨酸氨肽酶、焦谷氨酸氨肽酶或羧肽酶的影响。提取物的抑制作用以及对非肾上腺素能、非胆碱能神经刺激的抑制反应也不受蛋白酶抑制剂抑肽酶的影响。因此,活性物质不太可能是一种肽。7. 将提取物暴露于高碘酸或高碘酸钠会消除抑制活性。吡啶中的乙酸酐也会消除活性,但载体吡啶本身也有效果。8. 硼氢化钠而非硼酸盐在pH 2.0下添加到酸活化材料中时会消除抑制活性,但如果在pH 9.0下添加到稳定的无活性形式中则没有效果或甚至可能增强活性。当在pH 6.8下添加到酸活化但已中和的材料中时,它通常会消除抑制活性,但偶尔也没有效果。9. 这些结果表明这些提取物中的平滑肌抑制因子效力强大且可能是新的。它似乎不是一种肽或脂质,但可能含有碳水化合物作为分子的一部分。讨论了其可能的生理作用。

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