Porphyrins Regulate the Metabolic and Endocrine System: Role in Generation of Warburg Phenotype, Endogenous Digoxin Synthesis and Metabolic Syndrome X with Type 2 Diabetes Mellitus

A. Kurup, P. A. Kurup
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Porphyrins have been related to metabolic syndrome x and type 2 diabetes mellitus. The role of archaeal porphyrins in regulation of cell functions, metabolism and endocrine function is discussed. Porphyrins play a key role in the generation of the Warburg phenotype, endogenous digoxin synthesis and metabolic syndrome x with type 2 diabetes mellitus.  Methodology : The following groups were included in the study: - metabolic syndrome x with cerebrovascular thrombosis and coronary artery disease. There were 10 patients in each group and each patient had an age and sex matched healthy control selected randomly from the general population. The blood samples were drawn in the fasting state before treatment was initiated. Plasma from fasting heparinised blood was used and the experimental protocol was as follows (I) Plasma + phosphate buffered saline, (II) same as I + cholesterol substrate, (III) same as II + rutile 0.1 mg/ml, (IV) same as II + ciprofloxacine and doxycycline each in a concentration of 1 mg/ml. The following estimations were carried out: - Cytochrome F420, free RNA, free DNA, polycyclic aromatic hydrocarbon, hydrogen peroxide, pyruvate, ammonia, glutamate, succinate, glycine, delta aminolevulinic acid and digoxin. The study also involved estimating the following parameters in the patient population- hexokinase, porphyrins, pyruvate, glutamate, ammonia, succinic acid, serine, glycine, HMG CoA reductase, cytochrome C, blood ATP and heme oxygenase. Results : Plasma of control subjects showed increased levels of the above mentioned parameters with after incubation for 1 hour and addition of cholesterol substrate resulted in still further significant increase in these parameters. The plasma of patients showed similar results but the extent of increase was more. The addition of antibiotics to the control plasma caused a decrease in all the parameters while addition of rutile increased their levels. The addition of antibiotics and rutile to the patient’s plasma produced the same changes but the extent of change was more in patient’s sera as compared to controls. There was upregulated archaeal porphyrin synthesis in the patient population which was archaeal in origin as indicated by actinide catalysis of the reactions. The cholesterol oxidase pathway generated pyruvate which entered the GABA shunt pathway. This resulted in synthesis of succinate and glycine which are substrates for ALA synthase. The study showed the patient’s blood had increased heme oxygenase activity, increased serine, glycine, succinic acid and porphyrins. The hexokinase activity was high. The pyruvate, glutamate, ammonia, GABA and succinic acid levels were elevated indicating blockade of PDH activity, and operation of the GABA shunt pathway. The cytoC levels were increased in the serum indicating mitochondrial dysfunction suggested by low blood ATP levels. This was indicative of the Warburg’s phenotype. The HMG CoA reductase activity was high indicating cholesterol synthesis. The RHCD population had values similar to the patient population. The LHCD population had opposite values. Conclusion: An actinide dependent shadow biosphere of archaea and viroids in metabolic syndrome x with coronary and cerebrovascular diseases. The porphyrins can contribute to the pathogenesis of metabolic syndrome x with coronary and cerebrovascular diseases. Porphyrin synthesis is crucial in the pathogenesis of these disorders. Porphyrins may serve as regulatory molecules modulating immune, neural, endocrine, metabolic and genetic systems. The porphyrins photo-oxidation generated free radicals can produce immune activation, produce cell death, activate cell proliferation, produce insulin resistance and modulate conscious/quantal perception. Porphyrins can regulate hemispheric dominance. The archaeal porphyrins functions as key regulatory molecules with mitochondrial benzodiazepine receptors playing an important role. Key words : Actinide; Archaea; Porphyrins; GABA shunt; Peripheral benzodiazepine receptor; Delta aminolevulinic acid; Metabolic syndrome x; Type 2 diabetes mellitus; Coronary artery disease; Cerebrovascular disease","PeriodicalId":7348,"journal":{"name":"Advances in Natural Science","volume":null,"pages":null},"PeriodicalIF":0.0000,"publicationDate":"2012-09-26","publicationTypes":"Journal Article","fieldsOfStudy":null,"isOpenAccess":false,"openAccessPdf":"","citationCount":"0","resultStr":null,"platform":"Semanticscholar","paperid":null,"PeriodicalName":"Advances in Natural Science","FirstCategoryId":"1085","ListUrlMain":"https://doi.org/10.3968/J.ANS.1715787020120503.1073","RegionNum":0,"RegionCategory":null,"ArticlePicture":[],"TitleCN":null,"AbstractTextCN":null,"PMCID":null,"EPubDate":"","PubModel":"","JCR":"","JCRName":"","Score":null,"Total":0}
引用次数: 0

Abstract

Objectives : Actinidic archaea have been related to the pathogenesis of metabolic syndrome x. An actinide dependent shadow biosphere of archaea and viroids has been described in metabolic syndrome x with type 2 diabetes mellitus. Actinidic archaea have a mevalonate pathway and are cholesterol catabolizing. They can use cholesterol as a carbon and energy source. Archaeal cholesterol catabolism can generate porphyrins via the cholesterol ring oxidase generated pyruvate and GABA shunt pathway. Archaea can produce a secondary porphyria by inducing the enzyme heme oxygenase resulting in heme depletion and activation of the enzyme ALA synthase. Porphyrins have been related to metabolic syndrome x and type 2 diabetes mellitus. The role of archaeal porphyrins in regulation of cell functions, metabolism and endocrine function is discussed. Porphyrins play a key role in the generation of the Warburg phenotype, endogenous digoxin synthesis and metabolic syndrome x with type 2 diabetes mellitus.  Methodology : The following groups were included in the study: - metabolic syndrome x with cerebrovascular thrombosis and coronary artery disease. There were 10 patients in each group and each patient had an age and sex matched healthy control selected randomly from the general population. The blood samples were drawn in the fasting state before treatment was initiated. Plasma from fasting heparinised blood was used and the experimental protocol was as follows (I) Plasma + phosphate buffered saline, (II) same as I + cholesterol substrate, (III) same as II + rutile 0.1 mg/ml, (IV) same as II + ciprofloxacine and doxycycline each in a concentration of 1 mg/ml. The following estimations were carried out: - Cytochrome F420, free RNA, free DNA, polycyclic aromatic hydrocarbon, hydrogen peroxide, pyruvate, ammonia, glutamate, succinate, glycine, delta aminolevulinic acid and digoxin. The study also involved estimating the following parameters in the patient population- hexokinase, porphyrins, pyruvate, glutamate, ammonia, succinic acid, serine, glycine, HMG CoA reductase, cytochrome C, blood ATP and heme oxygenase. Results : Plasma of control subjects showed increased levels of the above mentioned parameters with after incubation for 1 hour and addition of cholesterol substrate resulted in still further significant increase in these parameters. The plasma of patients showed similar results but the extent of increase was more. The addition of antibiotics to the control plasma caused a decrease in all the parameters while addition of rutile increased their levels. The addition of antibiotics and rutile to the patient’s plasma produced the same changes but the extent of change was more in patient’s sera as compared to controls. There was upregulated archaeal porphyrin synthesis in the patient population which was archaeal in origin as indicated by actinide catalysis of the reactions. The cholesterol oxidase pathway generated pyruvate which entered the GABA shunt pathway. This resulted in synthesis of succinate and glycine which are substrates for ALA synthase. The study showed the patient’s blood had increased heme oxygenase activity, increased serine, glycine, succinic acid and porphyrins. The hexokinase activity was high. The pyruvate, glutamate, ammonia, GABA and succinic acid levels were elevated indicating blockade of PDH activity, and operation of the GABA shunt pathway. The cytoC levels were increased in the serum indicating mitochondrial dysfunction suggested by low blood ATP levels. This was indicative of the Warburg’s phenotype. The HMG CoA reductase activity was high indicating cholesterol synthesis. The RHCD population had values similar to the patient population. The LHCD population had opposite values. Conclusion: An actinide dependent shadow biosphere of archaea and viroids in metabolic syndrome x with coronary and cerebrovascular diseases. The porphyrins can contribute to the pathogenesis of metabolic syndrome x with coronary and cerebrovascular diseases. Porphyrin synthesis is crucial in the pathogenesis of these disorders. Porphyrins may serve as regulatory molecules modulating immune, neural, endocrine, metabolic and genetic systems. The porphyrins photo-oxidation generated free radicals can produce immune activation, produce cell death, activate cell proliferation, produce insulin resistance and modulate conscious/quantal perception. Porphyrins can regulate hemispheric dominance. The archaeal porphyrins functions as key regulatory molecules with mitochondrial benzodiazepine receptors playing an important role. Key words : Actinide; Archaea; Porphyrins; GABA shunt; Peripheral benzodiazepine receptor; Delta aminolevulinic acid; Metabolic syndrome x; Type 2 diabetes mellitus; Coronary artery disease; Cerebrovascular disease
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卟啉调节代谢和内分泌系统:在Warburg表型的产生、内源性地高辛合成和2型糖尿病代谢综合征X中的作用
目的:锕系古细菌与代谢综合征x的发病机制有关,在2型糖尿病合并代谢综合征x中发现了一个依赖锕系元素的古细菌和类病毒的阴影生物圈。放线菌具有甲羟戊酸途径和胆固醇分解代谢。它们可以利用胆固醇作为碳和能量的来源。古菌胆固醇分解代谢可通过胆固醇环氧化酶生成丙酮酸和GABA分流途径生成卟啉。古生菌可以通过诱导血红素加氧酶导致血红素耗竭和ALA合成酶激活而产生次生卟啉症。卟啉与代谢综合征x和2型糖尿病有关。讨论了古细菌卟啉在调节细胞功能、代谢和内分泌功能中的作用。卟啉在Warburg表型的产生、内源性地高辛合成和代谢综合征x伴2型糖尿病中起关键作用。方法:以下组被纳入研究:代谢综合征x合并脑血管血栓形成和冠状动脉疾病。每组有10名患者,每名患者从普通人群中随机选择年龄和性别匹配的健康对照。在治疗开始前,在禁食状态下抽取血样。使用空腹肝素化血血浆,实验方案如下:(I)血浆+磷酸盐缓冲盐水,(II)与I +胆固醇底物相同,(III)与II +金红石0.1 mg/ml相同,(IV)与II +环丙沙星和多西环素浓度均为1mg /ml相同。对细胞色素F420、游离RNA、游离DNA、多环芳烃、过氧化氢、丙酮酸、氨、谷氨酸、琥珀酸、甘氨酸、氨基乙酰丙酸和地高辛进行了估计。该研究还涉及估计患者人群中的以下参数-己糖激酶、卟啉、丙酮酸、谷氨酸、氨、琥珀酸、丝氨酸、甘氨酸、HMG辅酶a还原酶、细胞色素C、血液ATP和血红素加氧酶。结果:对照组在孵育1小时后,血浆中上述参数升高,添加胆固醇底物后,上述参数进一步显著升高。患者血浆也有类似结果,但升高幅度更大。在对照血浆中添加抗生素使各项指标均下降,而添加金红石使各项指标升高。在患者血浆中添加抗生素和金红石也产生了同样的变化,但与对照组相比,患者血清中的变化程度更大。古菌卟啉合成在患者群体中有上调,其来源是古菌,锕系元素催化反应表明。胆固醇氧化酶途径产生丙酮酸进入GABA分流途径。这导致琥珀酸盐和甘氨酸的合成,它们是ALA合酶的底物。研究表明,患者血液中的血红素加氧酶活性增加,丝氨酸、甘氨酸、琥珀酸和卟啉增加。己糖激酶活性高。丙酮酸、谷氨酸、氨、GABA和琥珀酸水平升高,表明PDH活性被阻断,GABA分流通路运行。血清中细胞c水平升高,提示低血ATP水平提示线粒体功能障碍。这表明了Warburg的表型。HMG CoA还原酶活性高,表明胆固醇合成。RHCD人群的值与患者人群相似。而LHCD人群的数值则相反。结论:代谢综合征合并冠状动脉和脑血管疾病中古细菌和类病毒存在锕系依赖的阴影生物圈。卟啉可能参与代谢综合征x合并冠状动脉和脑血管疾病的发病机制。卟啉合成在这些疾病的发病机制中起着至关重要的作用。卟啉可以作为调节分子调节免疫、神经、内分泌、代谢和遗传系统。卟啉光氧化产生的自由基可以产生免疫活化,产生细胞死亡,激活细胞增殖,产生胰岛素抵抗和调节意识/量子感知。卟啉可以调节半球优势。古细菌卟啉是线粒体苯二氮卓类受体的重要调控分子。关键词:锕系元素;古菌;卟啉;GABA分流;外周苯二氮卓受体;氨基乙酰丙酸;代谢综合征;2型糖尿病;冠状动脉疾病;脑血管疾病
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