Dihydropyridines

二氢吡啶
  • 文章类型: Journal Article
    迅速增加的高血压负担是心血管疾病(CVD)过早死亡的原因。肾脏疾病,和中风,巨大的公共卫生和财政负担。高血压检测,治疗,控制在世界范围内各不相同;它仍然很低,特别是在低收入和中等收入国家(LMICs)。高血压(BP)和CVD风险有很强,线性,独立协会。它们导致令人震惊的全因和CVD死亡人数。高血压增加的主要原因是交感神经活动,高血压的进一步并发症是心力衰竭,缺血性心脏病(IHD),中风,和肾衰竭。现在,抗高血压干预已成为降低BP相关发病率和死亡率的全球公共卫生优先事项.钙通道阻滞剂(CCB)是非常有效的血管扩张剂。以及用于控制高血压和CVD的最常见药物。西尼地平,同时具有L型和N型钙通道阻断活性,是一个很有前途的第四代建行。它通过L型钙通道阻滞引起血管舒张,并通过N型钙通道阻滞抑制交感神经系统(SNS)。西尼地平,作为双L/N型CCB,与氨氯地平相比,踏板水肿的发生率降低,仅阻断L型钙通道。西尼地平的抗高血压特性非常显著,具有低BP变异性和长效特性。对于高血压患者处理晨间高血压和由于过度的交感神经激活而导致夜间血压异常的患者是有益的。除了其降低BP的作用,它还通过交感神经抑制和肾素-血管紧张素-醛固酮系统抑制表现出器官保护作用;它控制心率和蛋白尿。保护雷诺,神经保护,西尼地平的心脏保护作用已得到充分记录和证明。
    The rapidly increasing burden of hypertension is responsible for premature deaths from cardiovascular disease (CVD), renal disease, and stroke, with a tremendous public health and financial burden. Hypertension detection, treatment, and control vary worldwide; it is still low, particularly in low- and middle-income countries (LMICs). High blood pressure (BP) and CVD risk have a strong, linear, and independent association. They contribute to alarming numbers of all-cause and CVD deaths. A major culprit for increased hypertension is sympathetic activity, and further complications of hypertension are heart failure, ischemic heart disease (IHD), stroke, and renal failure. Now, antihypertensive interventions have emerged as a global public health priority to reduce BP-related morbidity and mortality. Calcium channel blockers (CCB) are highly effective vasodilators. and the most common drugs used for managing hypertension and CVD. Cilnidipine, with both L- and N-type calcium channel blocking activity, is a promising 4th generation CCB. It causes vasodilation via L-type calcium channel blockade and inhibits the sympathetic nervous system (SNS) via N-type calcium channel blockade. Cilnidipine, which acts as a dual L/N-type CCB, is linked to a reduced occurrence of pedal edema compared to amlodipine, which solely blocks L-type calcium channels. The antihypertensive properties of cilnidipine are very substantial, with low BP variability and long-acting properties. It is beneficial for hypertensive patients to deal with morning hypertension and for patients with abnormal nocturnal BP due to exaggerated sympathetic nerve activation. Besides its BP-lowering effect, it also exhibits organ protection via sympathetic nerve inhibition and renin-angiotensin-aldosterone system inhibition; it controls heart rate and proteinuria. Reno-protective, neuroprotective, and cardioprotective effects of cilnidipine have been well-documented and demonstrated.
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