关于谷氨酸作用的神话和现实。现代世界文学科学资料汇编

Y. Paltov, Kh.P. Ivasivca, M. Pankiv
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One of the mechanisms of pathogenic effect of sodium glutamate is the contact local and free radical oxidizing effect on gastric tissues. In the oral route of administration of glutamate there are no phenomena of fat growth (obesity) as epidermal, which is characteristic of the abdominal form of obesity, so and pararectal, parallelic, pararenal and retroperitoneal, which is characteristic for the visceral form of obesity. In the subcutaneous and intraperitoneal routes of administration of glutamate in the neonatal period of life in experimental animals, glutamate causes hypersecretion of hydrochloric acid, the development of lesions manifested by hemorrhage, erosions and ulcers in the gastric mucosa and obesity. Prolonged administration of monosodium glutamate significantly enhances the striking effects of stress on the gastric mucosa. Morphological studies of the submandibular salivary glands of rats on the background of glutamate-induced obesity confirm the development of pathological changes, as evidenced by the detected vacuolar dystrophy in the acinar region, perivascular and periductal edema. On the background of abdominal obesity, dystrophic processes were found in the acinuses and minor dystrophic changes in the intraparticle inserts. Conclusion. In the subcutaneous and intraperitoneal routes of administration of glutamate in the neonatal period of life in experimental animals, glutamate causes hypersecretion of hydrochloric acid, the development of lesions manifested by hemorrhage, erosions and ulcers in the gastric mucosa and obesity. Prolonged administration of monosodium glutamate significantly enhances the striking effects of stress on the gastric mucosa. 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引用次数: 0

摘要

我们科学工作的目的是研究现有的谷氨酸对人体影响的实验模型,并了解这种影响的机制及其可能的后果。为了实现这一目标,我们研究了不同来源的科学医学文献。结果。在健康的身体中,谷氨酸作为一种神经递质,由大脑神经元分泌所需量的谷氨酸,参与人体的主要信息流。谷氨酸钠随着食物大量进入人体,影响人体,引起全身毒性作用,对胃、肠、唾液腺和胰腺等都有局部作用。根据科学文献,研究谷氨酸作用的实验模型分为口服谷氨酸进入体内的模型和新生儿期皮下和腹腔注射谷氨酸的模型。在第一种给药方式下,谷氨酸引起毒性作用,表现为血清中丙氨酸转氨酶、天冬氨酸转氨酶和γ -谷氨酰转肽酶的催化活性增高;1.6;而碱性磷酸酶活性保持在对照水平,表明谷氨酸钠作为膳食补充剂具有明显的肝毒性作用。引起血清中总肽和含酪氨酸肽含量增加,中、低分子量物质增多,中毒值升高,间接表明违反了实验动物肝脏内源性代谢物的解毒作用。在推荐剂量内摄入谷氨酸钠未显示引起胃壁粘膜、肌肉膜和浆膜的明显病理改变,但粘膜下膜血管有轻微充盈。已经发现,在高剂量下,谷氨酸钠对胃组织有局部致病作用,其表现为胃壁各层变薄,粘膜脱屑,并通过减小胃腺的大小、增加血管的数量和充血而使其解体。谷氨酸钠对胃组织的接触局部氧化和自由基氧化作用是其致病机制之一。在谷氨酸口服给药途径中,没有脂肪生长(肥胖)的表皮现象,这是腹部型肥胖的特征,也没有直肠旁、平行、肾旁和腹膜后的特征,这是内脏型肥胖的特征。在实验动物新生期皮下和腹腔给药谷氨酸的途径中,谷氨酸引起盐酸的高分泌,胃粘膜出血、糜烂、溃疡等病变的发展和肥胖。长期服用味精可显著增强应激对胃粘膜的显著影响。谷氨酸诱导肥胖大鼠下颌下唾液腺的形态学研究证实了其病理变化的发展,如腺泡区空泡营养不良、血管周围和导管周围水肿。在腹部肥胖的背景下,在腺泡中发现了营养不良的过程,在颗粒内插入物中发现了轻微的营养不良变化。结论。在实验动物新生期皮下和腹腔给药谷氨酸的途径中,谷氨酸引起盐酸的高分泌,胃粘膜出血、糜烂、溃疡等病变的发展和肥胖。长期服用味精可显著增强应激对胃粘膜的显著影响。谷氨酸诱导肥胖大鼠下颌下唾液腺的形态学研究证实了其病理变化的发展,如腺泡区空泡营养不良、血管周围和导管周围水肿。在腹部肥胖的背景下,在腺泡中发现了营养不良的过程,在颗粒内插入物中发现了轻微的营养不良变化。根据大量实验研究的结果和专业科学文献的报道,毫无疑问,在新生儿时期,谷氨酸引起的腹部肥胖只有通过皮下和腹腔给药途径才能发生,而口服给药方式则不会发生。
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Myths and reality about the effects of glutamate. Compilation of scientific data of modern world literature
The aim of our scientific work was to study the existing experimental models of glutamate effects on the body and to understand the mechanisms of this effect and its possible consequences. To achieve this goal, we have studied different sources of scientific medical literature. Results. In a healthy body, glutamic acid is secreted by brain neurons in the required amount as a neurotransmitter and participates in the main information flows of human body. Sodium glutamate, which enters the body with food in large quantities, affects the body, causing general toxic effects and has a local effect on the stomach, intestines, salivary glands and pancreas and so on. Based on the scientific literature, experimental models that study the effects of glutamate are divided into two types: models in which glutamate enters the body orally and when glutamate is administered subcutaneously and intraperitoneally in the neonatal period of life. In the first route of administration, glutamate causes a toxic effect, which is manifested in increased catalytic activity in the blood serum of alanine aminotransferase, aspartate aminotransferase and gamma-glutamyltranspeptidase in 2.5; 1.6; and 1.5 times, respectively, while the activity of alkaline phosphatase remained at control levels, indicating a pronounced hepatotoxic effect of monosodium glutamate as a dietary supplement. It causes an increase in content of total and tyrosine-containing peptides in the blood serum, increase of substances of low and medium molecular weight, as well as an increase in the values of intoxication, which indirectly indicates a violation of the detoxification of endogenous metabolites in the liver of experimental animals. Ingestion of sodium glutamate within the recommended doses has not been shown to cause marked pathological changes in the mucous, muscular and serous membranes of the gastric wall, but there is a slight fullness of the vessels of the submucosal membrane. It has been found that in high doses, sodium glutamate has a local pathogenic effect on the tissues of the stomach, which consists in thinning all layers of its wall, desquamation of the mucous membrane and its disorganization by reducing the size of gastric glands, increasing the number of vessels and their fullness with blood. One of the mechanisms of pathogenic effect of sodium glutamate is the contact local and free radical oxidizing effect on gastric tissues. In the oral route of administration of glutamate there are no phenomena of fat growth (obesity) as epidermal, which is characteristic of the abdominal form of obesity, so and pararectal, parallelic, pararenal and retroperitoneal, which is characteristic for the visceral form of obesity. In the subcutaneous and intraperitoneal routes of administration of glutamate in the neonatal period of life in experimental animals, glutamate causes hypersecretion of hydrochloric acid, the development of lesions manifested by hemorrhage, erosions and ulcers in the gastric mucosa and obesity. Prolonged administration of monosodium glutamate significantly enhances the striking effects of stress on the gastric mucosa. Morphological studies of the submandibular salivary glands of rats on the background of glutamate-induced obesity confirm the development of pathological changes, as evidenced by the detected vacuolar dystrophy in the acinar region, perivascular and periductal edema. On the background of abdominal obesity, dystrophic processes were found in the acinuses and minor dystrophic changes in the intraparticle inserts. Conclusion. In the subcutaneous and intraperitoneal routes of administration of glutamate in the neonatal period of life in experimental animals, glutamate causes hypersecretion of hydrochloric acid, the development of lesions manifested by hemorrhage, erosions and ulcers in the gastric mucosa and obesity. Prolonged administration of monosodium glutamate significantly enhances the striking effects of stress on the gastric mucosa. Morphological studies of the submandibular salivary glands of rats on the background of glutamate-induced obesity confirm the development of pathological changes, as evidenced by the detected vacuolar dystrophy in the acinar region, perivascular and periductal edema. On the background of abdominal obesity, dystrophic processes were found in the acinuses and minor dystrophic changes in the intraparticle inserts. There is no doubt in the fact, which is based on the results of numerous experimental studies and covered in professional scientific litefrature, that the abdominal form of glutamate-induced obesity is possible only with subcutaneous and intraperitoneal routes of its administration in the neonatal period of life and while intraorall way of administration does not occur.
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