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首页> 外文期刊>Virology >Efficient repeated low-dose intravaginal infection with X4 and R5 SHIVs in rhesus macaque: Implications for HIV-1 transmission in humans
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Efficient repeated low-dose intravaginal infection with X4 and R5 SHIVs in rhesus macaque: Implications for HIV-1 transmission in humans

机译:恒河猴中X4和R5 SHIV的有效反复小剂量阴道内感染:对人类HIV-1传播的影响

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We examined the effect of inoculum dose on SHIV transmission and infection. We found that repeated low-dose intravaginal exposure with either R5-SHIVSF162P3 or X4-SFIVSF33A results in infections that are blunted and rapidly controlled. Interestingly, although the transmission rate after all repeated exposures is comparable for the two viruses, the probability of low-dose vaginal transmission is greater for the X4 than R5 virus. Furthermore, X4-SHIVSF33A replication predominates in low-dose dually-exposed macaques, suggesting that it is better at establishing a systemic infection following transmission. However, X4-SHIVSF33A advantage in transmission and infection is not observed in macaques inoculated intravenously with low-dose mixed inoculum. The finding that although matched in tissue culture infectious dose, the X4 inoculum is more complex leads us to hypothesize that the greater genetic heterogeneity of the X4 virus population may have rendered it less susceptible to the severe bottleneck effects imposed by IVAG inoculation with small doses, allowing for greater probability of transmission and establishment of a generalized infection. These data have implications for HIV-1 transmission and infection in humans. (C) 2006 Elsevier Inc. All rights reserved.
机译:我们检查了接种剂量对SHIV传播和感染的影响。我们发现,反复使用R5-SHIVSF162P3或X4-SFIVSF33A进行低剂量阴道内暴露会导致感染变钝并迅速得到控制。有趣的是,尽管两种病毒在所有重复接触后的传播率均相当,但X4的低剂量阴道传播的可能性要大于R5病毒。此外,X4-SHIVSF33A复制在低剂量双重暴露的猕猴中占主导地位,这表明它在传播后建立全身性感染方面更好。但是,X4-SHIVSF33A在传播和感染方面的优势在以小剂量混合接种物静脉注射的猕猴中未观察到。 X4接种物虽然与组织培养的感染剂量相匹配,但更复杂,这一发现使我们推测X4病毒种群的更大遗传异质性可能使其对小剂量IVAG接种所造成的严重瓶颈效应的敏感性降低,可以更大程度地传播和建立全身感染。这些数据对HIV-1在人类的传播和感染有影响。 (C)2006 Elsevier Inc.保留所有权利。

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