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膦甲酸钠。对其在免疫功能低下的巨细胞病毒性视网膜炎患者中的抗病毒活性、药代动力学特性及治疗应用的综述。

Foscarnet. A review of its antiviral activity, pharmacokinetic properties and therapeutic use in immunocompromised patients with cytomegalovirus retinitis.

作者信息

Chrisp P, Clissold S P

机构信息

Adis Drug Information Services, Auckland, New Zealand.

出版信息

Drugs. 1991 Jan;41(1):104-29. doi: 10.2165/00003495-199141010-00009.

Abstract

The pyrophosphate analogue, foscarnet, selectively inhibits the DNA polymerase of human herpes viruses, including cytomegalovirus, and the reverse transcriptase of HIV. Viral replication is therefore prevented, but resumes when the drug is cleared from infected cells. In vitro, the combination of foscarnet and zidovudine (azidothymidine) has an additive effect against cytomegalovirus and acts synergistically against HIV. An improvement in cytomegalovirus retinitis is obtained in over 85% of affected AIDS patients during foscarnet induction therapy, but relapse usually occurs within a month of ceasing treatment. There is a similar duration of remission during maintenance therapy given for 5 days each week, but this can be extended 4- to 5-fold with daily administration of higher doses. In allograft recipients, progression of retinitis can be halted by foscarnet until immune function recovers and eradicates the virus. The incidence of acute renal failure, which is common during foscarnet therapy, may be reduced by dosage adjustment and adequate prehydration. Anaemia, phlebitis, nausea and vomiting, and disturbances in serum calcium and phosphate levels, perhaps resulting from uptake of foscarnet into bone or chelation with ionised calcium, have also been associated with administration of the drug. Cytomegalovirus retinitis is difficult to treat, with few therapeutic options available. Although treatment with foscarnet produces some severe adverse effects, with care these can be minimised, and the drug produces clinical improvement in a large proportion of patients; this is a highly encouraging finding at this stage in its development. Preliminary comparative data indicate that foscarnet and ganciclovir are similarly effective, but foscarnet may have some theoretical advantages in AIDS patients since it can be used in combination with zidovudine without potentiating myelosuppression.

摘要

焦磷酸盐类似物膦甲酸钠可选择性抑制人类疱疹病毒(包括巨细胞病毒)的DNA聚合酶以及HIV的逆转录酶。因此可阻止病毒复制,但当药物从受感染细胞中清除后,病毒复制会恢复。在体外,膦甲酸钠与齐多夫定(叠氮胸苷)联合使用对巨细胞病毒有相加作用,对HIV有协同作用。在膦甲酸钠诱导治疗期间,超过85%的患巨细胞病毒性视网膜炎的艾滋病患者病情得到改善,但通常在停止治疗后一个月内复发。每周给药5天进行维持治疗时缓解期持续时间相似,但每日给予更高剂量可将缓解期延长4至5倍。在同种异体移植受者中,膦甲酸钠可阻止视网膜炎进展,直至免疫功能恢复并清除病毒。膦甲酸钠治疗期间常见的急性肾衰竭发生率可通过调整剂量和充分的水化预处理来降低。贫血、静脉炎、恶心和呕吐以及血清钙和磷水平紊乱,可能是由于膦甲酸钠进入骨骼或与离子钙螯合所致,也与该药物的使用有关。巨细胞病毒性视网膜炎难以治疗,可用的治疗选择很少。虽然膦甲酸钠治疗会产生一些严重不良反应,但谨慎使用可将这些不良反应降至最低,并且该药物可使大部分患者的病情得到临床改善;在其研发的现阶段,这是一个非常令人鼓舞的发现。初步比较数据表明,膦甲酸钠和更昔洛韦疗效相似,但膦甲酸钠在艾滋病患者中可能具有一些理论优势,因为它可与齐多夫定联合使用而不会增强骨髓抑制作用。

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