西洛他唑:环核苷酸磷酸二酯酶3型和腺苷摄取的双重抑制剂。

Yongge Liu, Y. Shakur, M. Yoshitake, J. Kambayashi
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引用次数: 180

摘要

西洛他唑(Pletal)是一种喹诺啉酮衍生物,自1999年以来在美国被批准用于治疗间歇性跛行(IC)症状,自1988年以来在日本和其他亚洲国家被批准用于相关适应症。西洛他唑的血管扩张和抗血小板作用主要是由于抑制磷酸二酯酶3 (PDE3)和随后的细胞内cAMP水平升高。最近的临床前研究表明,西洛他唑还具有抑制腺苷摄取的能力,这一特性可能将其与其他PDE3抑制剂(如米力酮)区分开来。西洛他唑可提高间质和循环腺苷水平,增强血小板和平滑肌中PDE3抑制的camp升高作用,从而增强药物的抗血小板和血管舒张作用。相反,西洛他唑升高心脏间质腺苷已被证明可降低西洛他唑抑制pde3作用引起的cAMP升高,从而减弱其强心作用。据报道,西洛他唑还能在体外抑制平滑肌细胞增殖,并在一项临床研究中被证明有利于改变血浆脂质:降低甘油三酯和增加高密度脂蛋白胆固醇水平。这些作用中的一种或几种作用的组合可能有助于该药在IC和其他继发于动脉粥样硬化的疾病条件下的临床益处和安全性。在8项双盲随机安慰剂对照试验中,西洛他唑显著增加了跑步机上的最大步行距离或绝对跛行距离。此外,西洛他唑改善了患者问卷调查的生活质量指标。一项大型随机、双盲、安慰剂对照、多中心竞争试验表明,西洛他唑优于己酮茶碱(另一种批准用于IC的药物)。西洛他唑通常耐受性良好,最常见的不良事件是头痛、腹泻、大便异常和头晕。最近也有关于西洛他唑用于预防冠状动脉血栓形成/再狭窄和中风复发的研究报道。
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Cilostazol (pletal): a dual inhibitor of cyclic nucleotide phosphodiesterase type 3 and adenosine uptake.
Cilostazol (Pletal), a quinolinone derivative, has been approved in the U.S. for the treatment of symptoms of intermittent claudication (IC) since 1999 and for related indications since 1988 in Japan and other Asian countries. The vasodilatory and antiplatelet actions of cilostazol are due mainly to the inhibition of phosphodiesterase 3 (PDE3) and subsequent elevation of intracellular cAMP levels. Recent preclinical studies have demonstrated that cilostazol also possesses the ability to inhibit adenosine uptake, a property that may distinguish it from other PDE3 inhibitors, such as milrinone. Elevation of interstitial and circulating adenosine levels by cilostazol has been found to potentiate the cAMP-elevating effect of PDE3 inhibition in platelets and smooth muscle, thereby augmenting antiplatelet and vasodilatory effects of the drug. In contrast, elevation of interstitial adenosine by cilostazol in the heart has been shown to reduce increases in cAMP caused by the PDE3-inhibitory action of cilostazol, thus attenuating the cardiotonic effects. Cilostazol has also been reported to inhibit smooth muscle cell proliferation in vitro and has been demonstrated in a clinical study to favorably alter plasma lipids: to decrease triglyceride and to increase HDL-cholesterol levels. One, or a combination of several of these effects may contribute to the clinical benefits and safety of this drug in IC and other disease conditions secondary to atherosclerosis. In eight double-blind randomized placebo-controlled trials, cilostazol significantly increased maximal walking distance, or absolute claudication distance on a treadmill. In addition, cilostazol improved quality of life indices as assessed by patient questionnaire. One large randomized, double-blinded, placebo-controlled, multicenter competitor trial demonstrated the superiority of cilostazol over pentoxifylline, the only other drug approved for IC. Cilostazol has been generally well-tolerated, with the most common adverse events being headache, diarrhea, abnormal stools and dizziness. Studies involving off-label use of cilostazol for prevention of coronary thrombosis/restenosis and stroke recurrence have also recently been reported.
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