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首页> 外文期刊>Journal of Cachexia, Sarcopenia and Muscle >Cardio‐renal cachexia syndromes (CRCS): pathophysiological foundations of a vicious pathological circle
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Cardio‐renal cachexia syndromes (CRCS): pathophysiological foundations of a vicious pathological circle

机译:心肾恶病质综合征(CRCS):恶性病理循环的病理生理基础

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AbstractCardio-renal syndromes (CRS) are defined as disorders of the heart and kidney whereby acute or chronic dysfunction in one organ may induce acute or chronic dysfunction of the other. CRS have been classified into five categories, where types 2 and 4 represent respectively chronic cardio-renal and chronic reno-cardiac syndromes. In these conditions, the chronic disorder of either the heart or kidney has been shown to induce some degree of cachexia. At the same time, cachexia has been proposed as a possible mechanism contributing to the worsening of such pathological organ cross talk. Common pathogenetic mechanisms underlie body wasting in cachectic states of different chronic heart and kidney diseases. In these circumstances, a vicious circle could arise, in which cachexia associated with either heart failure or chronic kidney disease may contribute to further damage of the other organ. In chronic CRS, activation of the immune and neuroendocrine systems contributes to the genesis of cachexia, which in turn can negatively affect the heart and kidney function. In patients with cardiac sustained activation of the immune and neuroendocrine systems and oxidative stress, renal vascular resistance can increase and therefore impair renal perfusion, leading to worsening kidney function. Similarly, in renal cachexia, increased levels of pro-inflammatory cytokines can cause progressive left ventricular systolic dysfunction, myocardial cell death, endothelial dysfunction and increased myocardial fibrosis, with consequent impairment of the chronic reno-cardiac syndrome type 4. Thus, we speculate that the occurrence of different types of chronic CRS could represent a fundamental step in the genesis of cachexia, being renal and cardiac dysfunction closely related to the occurrence of systemic disorders leading to a final common pathway. Therefore, the heart and kidney and cachexia represent a triad causing a vicious circle that increases mortality and morbidity: In such circumstances, we may plausibly talk about cardio-renal cachexia syndrome. Complex interrelations may explain the transition from CRS to cachexia and from cachexia to CRS. Identification of the exact mechanisms occurring in these conditions could potentially help in preventing and treating this deadly combination.
机译:摘要心脏肾综合征(CRS)定义为心脏和肾脏的疾病,由此一个器官的急性或慢性功能障碍可能诱发另一器官的急性或慢性功能障碍。 CRS已分为五类,其中2型和4型分别代表慢性心肾综合征和慢性肾心综合征。在这些情况下,心脏或肾脏的慢性疾病已显示出一定程度的恶病质。同时,恶病质已被提出作为导致这种病理器官串扰恶化的可能机制。常见的致病机制是人体在不同慢性心脏病和肾脏疾病的恶病质状态下消瘦的基础。在这些情况下,可能会形成恶性循环,其中与心力衰竭或慢性肾脏疾病相关的恶病质可能会进一步损害其他器官。在慢性CRS中,免疫系统和神经内分泌系统的激活有助于恶病质的发生,而恶病质又会负面影响心脏和肾脏的功能。在心脏免疫系统和神经内分泌系统持续激活且氧化应激的患者中,肾血管阻力会增加,从而损害肾灌注,从而导致肾功能恶化。同样,在肾脏恶病质中,促炎性细胞因子水平升高可导致进行性左心室收缩功能障碍,心肌细胞死亡,内皮功能障碍和心肌纤维化增加,从而损害4型慢性肾病性心脏病。不同类型的慢性CRS的发生可能代表恶病质的发生的基本步骤,因为肾脏和心脏功能障碍与导致最终共同途径的全身性疾病的发生密切相关。因此,心脏,肾脏和恶病质代表一个三元组,引起恶性循环,从而增加死亡率和发病率:在这种情况下,我们可能会谈论心肾恶病质综合征。复杂的相互关系可以解释从CRS到恶病质以及从恶病质到CRS的过渡。确定在这些情况下发生的确切机制可能有助于预防和治疗这种致命的组合。

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