The Extinction of Homo Sapiens and Symbiotic Neanderthalisation: Relation to Archaeal Mediated RNA Viroidsand Amyloidosis

R. Kurup, P. A. Kurup
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This abnormal protein resists digestion by lysosomal enzymes after its half-life is over and results in deposition of amyloid plaques. This produces organ dysfunction. Prion phenomena were initially described for Creutzfeldt Jakob’s disease, but now it is found to be wide spread in chronic disease pathogenesis. Ribonucleoproteins are well known to behave like prion proteins and form amyloid. We have demonstrated actinidic archaea which secretes RNA viroids in metabolic syndrome, neurodegenerations, cancer, autoimmune disease, schizophrenia, autism and CJD. The RNA viroids can bind with normal proteins with prion like domains eg., superoxide dismutase and produce a ribonucleoprotein resulting in prion phenomena and amyloidogenesis. Materials and Methods: The following groups were included in the study:- alzheimer’s disease, multiple sclerosis, non-hodgkin’s lymphoma, metabolic syndrome x with cerebrovascular thrombosis and coronary artery disease, schizophrenia, autism, seizure disorder, creutzfeldt jakob disease and acquired immunodeficiency syndrome. 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+cerium 0.1 mg/ml, (IV) same as II+ciprofloxacine and doxycycline each in a concentration of 1 mg/ml. Cholesterol substrate was prepared as described by Richmond. Aliquots were withdrawn at zero time immediately after mixing and after incubation at 37oC for 1 hour. The following estimations were carried out:- Cytochrome F420, free RNA, Cytochrome F420 was estimated flourimetrically (excitation wavelength 420 nm and emission wavelength 520 nm). 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 cerium increased their levels. The addition of antibiotics to the patient’s plasma caused a decrease in all the parameters while addition of cerium increased their levels but the extent of change was more in patient’s sera as compared to controls. Discussion: The actinidic archaeal growth results in increased digoxin synthesis and phenotypic conversion of homo sapiens to homo Neanderthals as reported earlier. The increased actinidic archaeal growth is due to global warming and these results in neanderthalisation.Homo neanderthalis tend to have more of civilisational diseases like metabolic syndrome, neurodegenerations, cancer, autoimmune disease, schizophrenia, autism and CJD. Actinidic archaeal secreted RNA viroids may play a crucial role in amyloid formation and pathogenesis of these disorders. The evolution and origin of homo sapiens and homo neanderthalis is on the basis of actinidic archaeal symbiosis and digoxin synthesis. Extreme climate change related increased actinidic archaeal symbiosis and digoxin synthesis results in homo neanderthalis. The homo sapien species results from inhibition of actinidic archaeal symbiosis and endogenous digoxin synthesis by normal global climate. Thus there are evolutionary swings between the two human species depending on extremes of climate and archaeal symbiosis. Endogenous digoxin can be considered as a Neanderthal hormone. The results show that there was increase in cytochrome F420 in CJD and other disease groups indicating increased archaeal growth. There was also an increase in free RNA indicating self-replicating RNA viroids in CJD and other disease groups. The RNA viroid generation was catalysed by actinides. The RNA viroids can bind with proteins having prion like domains forming ribonucleoproteins. These ribonucleoproteins can give an abnormal conformation to the protein resulting in generation of abnormal prions. The abnormal prions can act as a template to convert normal proteins with normal configuration to abnormal conformation. This can result in amyloidogenesis. The abnormal configured proteins will resist lysosomal digestion and accumulate as amyloid producing disease states and extinction.","PeriodicalId":7348,"journal":{"name":"Advances in Natural Science","volume":null,"pages":null},"PeriodicalIF":0.0000,"publicationDate":"2014-06-26","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/10.3968/4381","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

Introduction: Prion proteins have been implicated in systemic disorders like neurodegenerations, cancer and metabolic syndrome. The beta amyloid in Alzheimer’s disease, alpha synuclein in parkinson’s disease, the TAR protein in frontotemporal dementia and copper zinc dismutase in motor neuron disease behaves like prion proteins. Prion proteins like behavior is also seen in the tumour suppressor P53 protein in cancer and the islet cell associated amyloid in diabetes mellitus. Prion diseases are conformational diseases. The abnormal prion protein seeded into the system converts the normal proteins with prion like domains to abnormal configuration. This abnormal protein resists digestion by lysosomal enzymes after its half-life is over and results in deposition of amyloid plaques. This produces organ dysfunction. Prion phenomena were initially described for Creutzfeldt Jakob’s disease, but now it is found to be wide spread in chronic disease pathogenesis. Ribonucleoproteins are well known to behave like prion proteins and form amyloid. We have demonstrated actinidic archaea which secretes RNA viroids in metabolic syndrome, neurodegenerations, cancer, autoimmune disease, schizophrenia, autism and CJD. The RNA viroids can bind with normal proteins with prion like domains eg., superoxide dismutase and produce a ribonucleoprotein resulting in prion phenomena and amyloidogenesis. Materials and Methods: The following groups were included in the study:- alzheimer’s disease, multiple sclerosis, non-hodgkin’s lymphoma, metabolic syndrome x with cerebrovascular thrombosis and coronary artery disease, schizophrenia, autism, seizure disorder, creutzfeldt jakob disease and acquired immunodeficiency syndrome. 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+cerium 0.1 mg/ml, (IV) same as II+ciprofloxacine and doxycycline each in a concentration of 1 mg/ml. Cholesterol substrate was prepared as described by Richmond. Aliquots were withdrawn at zero time immediately after mixing and after incubation at 37oC for 1 hour. The following estimations were carried out:- Cytochrome F420, free RNA, Cytochrome F420 was estimated flourimetrically (excitation wavelength 420 nm and emission wavelength 520 nm). 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 cerium increased their levels. The addition of antibiotics to the patient’s plasma caused a decrease in all the parameters while addition of cerium increased their levels but the extent of change was more in patient’s sera as compared to controls. Discussion: The actinidic archaeal growth results in increased digoxin synthesis and phenotypic conversion of homo sapiens to homo Neanderthals as reported earlier. The increased actinidic archaeal growth is due to global warming and these results in neanderthalisation.Homo neanderthalis tend to have more of civilisational diseases like metabolic syndrome, neurodegenerations, cancer, autoimmune disease, schizophrenia, autism and CJD. Actinidic archaeal secreted RNA viroids may play a crucial role in amyloid formation and pathogenesis of these disorders. The evolution and origin of homo sapiens and homo neanderthalis is on the basis of actinidic archaeal symbiosis and digoxin synthesis. Extreme climate change related increased actinidic archaeal symbiosis and digoxin synthesis results in homo neanderthalis. The homo sapien species results from inhibition of actinidic archaeal symbiosis and endogenous digoxin synthesis by normal global climate. Thus there are evolutionary swings between the two human species depending on extremes of climate and archaeal symbiosis. Endogenous digoxin can be considered as a Neanderthal hormone. The results show that there was increase in cytochrome F420 in CJD and other disease groups indicating increased archaeal growth. There was also an increase in free RNA indicating self-replicating RNA viroids in CJD and other disease groups. The RNA viroid generation was catalysed by actinides. The RNA viroids can bind with proteins having prion like domains forming ribonucleoproteins. These ribonucleoproteins can give an abnormal conformation to the protein resulting in generation of abnormal prions. The abnormal prions can act as a template to convert normal proteins with normal configuration to abnormal conformation. This can result in amyloidogenesis. The abnormal configured proteins will resist lysosomal digestion and accumulate as amyloid producing disease states and extinction.
智人的灭绝和共生的尼安德特人化:与古细菌介导的RNA类病毒和淀粉样变性的关系
导言:朊蛋白与神经退行性疾病、癌症和代谢综合征等全身性疾病有关。阿尔茨海默病中的β淀粉样蛋白、帕金森病中的α突触核蛋白、额颞叶痴呆中的TAR蛋白和运动神经元疾病中的铜锌歧化酶的行为与朊病毒蛋白类似。类似朊蛋白的行为也见于癌症的肿瘤抑制蛋白P53和糖尿病的胰岛细胞相关淀粉样蛋白。朊病毒疾病是构象性疾病。植入系统的异常朊病毒蛋白将具有朊病毒样结构域的正常蛋白转化为异常结构。这种异常蛋白在其半衰期结束后抵抗溶酶体酶的消化,并导致淀粉样斑块的沉积。这会导致器官功能障碍。朊病毒现象最初被描述为克雅氏病,但现在发现它在慢性疾病发病机制中广泛存在。众所周知,核糖核蛋白的行为与朊蛋白相似,并形成淀粉样蛋白。我们已经证明在代谢综合征,神经变性,癌症,自身免疫性疾病,精神分裂症,自闭症和CJD中分泌RNA类病毒的放线性古菌。RNA类病毒可以与具有朊病毒样结构域的正常蛋白质结合。,超氧化物歧化酶和产生核糖核蛋白导致朊病毒现象和淀粉样蛋白的形成。材料与方法:本研究纳入以下组:阿尔茨海默病、多发性硬化、非霍奇金淋巴瘤、代谢综合征x伴脑血管血栓形成和冠状动脉疾病、精神分裂症、自闭症、癫痫发作障碍、克雅氏病和获得性免疫缺陷综合征。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+cerium 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。按照Richmond的描述制备胆固醇底物。在混合和37℃孵育1小时后,立即在零时间取出等分。细胞色素F420,游离RNA,荧光法测定细胞色素F420(激发波长420 nm,发射波长520 nm)。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参数均降低,而添加铈使各参数均升高。在患者血浆中添加抗生素导致所有参数下降,而添加铈使其水平升高,但患者血清中的变化程度比对照组更大。讨论:如前所述,锕系古细菌的生长导致地高辛合成的增加和智人向尼安德特人的表型转化。锕系古细菌增长的增加是由于全球变暖和尼安德特人化的结果。尼安德特人往往有更多的文明疾病,如代谢综合征、神经变性、癌症、自身免疫性疾病、精神分裂症、自闭症和克雅氏病。锕系古菌分泌的RNA类病毒可能在淀粉样蛋白的形成和这些疾病的发病机制中起关键作用。智人和尼安德特人的进化和起源是基于锕系古菌共生和地高辛合成。极端气候变化与尼安德特人锕系古细菌共生和地高辛合成的增加有关。正常的全球气候抑制了锕系古细菌的共生和内源性地高辛的合成,从而形成了智人。因此,根据极端的气候和古菌共生关系,这两个人类物种之间存在着进化的波动。内源性地高辛可以被认为是尼安德特人的激素。结果显示,CJD和其他疾病组细胞色素F420增加,表明古菌生长增加。在CJD和其他疾病组中,自由RNA也有所增加,表明存在自我复制的RNA类病毒。RNA类病毒的生成是由锕系元素催化的。RNA类病毒可以与具有朊病毒样结构域的蛋白质结合形成核糖核蛋白。这些核糖核蛋白可以使蛋白质产生异常构象,从而产生异常朊病毒。
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