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本文引用的文献

1
Impact of inhalation exposure modality and particle size on the respiratory deposition of ricin in BALB/c mice.吸入暴露方式和颗粒大小对蓖麻毒素在BALB/c小鼠呼吸道沉积的影响。
Inhal Toxicol. 2003 May;15(6):619-38. doi: 10.1080/08958370390205092.
2
Potential antiviral therapeutics for smallpox, monkeypox and other orthopoxvirus infections.针对天花、猴痘及其他正痘病毒感染的潜在抗病毒疗法。
Antiviral Res. 2003 Jan;57(1-2):13-23. doi: 10.1016/s0166-3542(02)00196-1.
3
Role of cidofovir in the treatment of DNA virus infections, other than CMV infections, in immunocompromised patients.西多福韦在免疫功能低下患者中治疗除巨细胞病毒感染以外的DNA病毒感染中的作用。
Curr Opin Investig Drugs. 2002 Nov;3(11):1561-6.
4
Cidofovir in the therapy and short-term prophylaxis of poxvirus infections.西多福韦用于痘病毒感染的治疗和短期预防。
Trends Pharmacol Sci. 2002 Oct;23(10):456-8. doi: 10.1016/s0165-6147(02)02091-6.
5
Cidofovir in the treatment of poxvirus infections.西多福韦治疗痘病毒感染
Antiviral Res. 2002 Jul;55(1):1-13. doi: 10.1016/s0166-3542(02)00008-6.
6
Treatment of aerosolized cowpox virus infection in mice with aerosolized cidofovir.用雾化西多福韦治疗小鼠雾化牛痘病毒感染
Antiviral Res. 2002 Jun;54(3):129-42. doi: 10.1016/s0166-3542(01)00220-0.
7
Characterization of wild-type and cidofovir-resistant strains of camelpox, cowpox, monkeypox, and vaccinia viruses.骆驼痘病毒、牛痘病毒、猴痘病毒和痘苗病毒野生型及西多福韦耐药株的特性分析
Antimicrob Agents Chemother. 2002 May;46(5):1329-35. doi: 10.1128/AAC.46.5.1329-1335.2002.
8
Effects of cidofovir on the pathogenesis of a lethal vaccinia virus respiratory infection in mice.西多福韦对小鼠致死性痘苗病毒呼吸道感染发病机制的影响。
Antiviral Res. 2001 Oct;52(1):55-62. doi: 10.1016/s0166-3542(01)00159-0.
9
Expression of mouse interleukin-4 by a recombinant ectromelia virus suppresses cytolytic lymphocyte responses and overcomes genetic resistance to mousepox.重组埃可病毒表达小鼠白细胞介素-4可抑制细胞溶解性淋巴细胞反应并克服对鼠痘的遗传抗性。
J Virol. 2001 Feb;75(3):1205-10. doi: 10.1128/JVI.75.3.1205-1210.2001.
10
Inhaled zanamivir for the prevention of influenza in families. Zanamivir Family Study Group.吸入扎那米韦预防家庭内流感。扎那米韦家庭研究小组。
N Engl J Med. 2000 Nov 2;343(18):1282-9. doi: 10.1056/NEJM200011023431801.

雾化的西多福韦保留在呼吸道中,并保护小鼠免受鼻内接种的牛痘病毒攻击。

Aerosolized cidofovir is retained in the respiratory tract and protects mice against intranasal cowpox virus challenge.

作者信息

Roy Chad J, Baker Robert, Washburn Kenneth, Bray Mike

机构信息

Department of Aerobiology and Product Evaluation, US Army Medical Research Institute of Infectious Diseases, Fort Detrick, Maryland 21702, USA.

出版信息

Antimicrob Agents Chemother. 2003 Sep;47(9):2933-7. doi: 10.1128/AAC.47.9.2933-2937.2003.

DOI:10.1128/AAC.47.9.2933-2937.2003
PMID:12936997
原文链接:https://pmc.ncbi.nlm.nih.gov/articles/PMC182607/
Abstract

We employed a murine model to test the concept of using an aerosolized, long-acting antiviral drug to protect humans against smallpox. We previously showed that a low dose of aerosolized cidofovir (HPMPC [Vistide]) was highly protective against subsequent aerosolized cowpox virus challenge and was more effective than a much larger dose of drug given by injection, suggesting that aerosolized cidofovir is retained in the lung. Because the nephrotoxicity of cidofovir is a major concern in therapy, delivering the drug directly to the respiratory tract might be an effective prophylactic strategy that maximizes the tissue concentration at the site of initial viral replication, while minimizing its accumulation in the kidneys. In the present study, we found that treating mice with aerosolized (14)C-labeled cidofovir ((14)C-cidofovir) resulted in the prolonged retention of radiolabeled drug in the lungs at levels greatly exceeding those in the kidneys. In contrast, subcutaneous injection produced much higher concentrations of (14)C-cidofovir in the kidneys than in the lungs over the 96-h time course of the study. As further evidence of the protective efficacy of aerosolized cidofovir, we found that aerosol treatment before or after infection was highly protective in mice challenged intranasally with cowpox virus. All or nearly all mice that were treated once by aerosol, from 2 days before to 2 days after challenge, survived intranasal infection, whereas all placebo-treated animals died.

摘要

我们采用了一种小鼠模型来测试使用雾化长效抗病毒药物保护人类免受天花感染这一概念。我们之前表明,低剂量雾化西多福韦(HPMPC [Vistide])对随后雾化牛痘病毒攻击具有高度保护作用,且比大得多的注射剂量药物更有效,这表明雾化西多福韦可保留在肺部。由于西多福韦的肾毒性是治疗中的主要问题,将药物直接递送至呼吸道可能是一种有效的预防策略,可使初始病毒复制部位的组织浓度最大化,同时将其在肾脏中的蓄积最小化。在本研究中,我们发现用雾化的(14)C标记西多福韦((14)C - 西多福韦)治疗小鼠会导致放射性标记药物在肺部长期保留,其水平大大超过在肾脏中的水平。相比之下,在研究的96小时时间进程中,皮下注射产生的(14)C - 西多福韦在肾脏中的浓度比在肺部高得多。作为雾化西多福韦保护功效的进一步证据,我们发现感染前或感染后进行雾化治疗对经鼻接种牛痘病毒攻击的小鼠具有高度保护作用。从攻击前2天到攻击后2天接受一次雾化治疗的所有或几乎所有小鼠均在鼻内感染中存活,而所有接受安慰剂治疗的动物均死亡。