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携带Mx1流感病毒抗性基因的小鼠对严重流感病毒感染的抵抗力很大程度上取决于遗传背景。

Protection from Severe Influenza Virus Infections in Mice Carrying the Mx1 Influenza Virus Resistance Gene Strongly Depends on Genetic Background.

作者信息

Shin Dai-Lun, Hatesuer Bastian, Bergmann Silke, Nedelko Tatiana, Schughart Klaus

机构信息

Department of Infection Genetics, Helmholtz Centre for Infection Research, Braunschweig, Germany University of Veterinary Medicine Hannover, Hannover, Germany.

University of Tennessee Health Science Center, Memphis, Tennessee, USA.

出版信息

J Virol. 2015 Oct;89(19):9998-10009. doi: 10.1128/JVI.01305-15. Epub 2015 Jul 22.

Abstract

UNLABELLED

Influenza virus infections represent a serious threat to human health. Both extrinsic and intrinsic factors determine the severity of influenza. The MX dynamin-like GTPase 1 (Mx1) gene has been shown to confer strong resistance to influenza A virus infections in mice. Most laboratory mouse strains, including C57BL/6J, carry nonsense or deletion mutations in Mx1 and thus a nonfunctional allele, whereas wild-derived mouse strains carry a wild-type Mx1 allele. Congenic C57BL/6J (B6-Mx1(r/r)) mice expressing a wild-type allele from the A2G mouse strain are highly resistant to influenza A virus infections, to both mono- and polybasic subtypes. Furthermore, in genetic mapping studies, Mx1 was identified as the major locus of resistance to influenza virus infections. Here, we investigated whether the Mx1 protective function is influenced by the genetic background. For this, we generated a congenic mouse strain carrying the A2G wild-type Mx1 resistance allele on a DBA/2J background (D2-Mx1(r/r)). Most remarkably, congenic D2-Mx1(r/r) mice expressing a functional Mx1 wild-type allele are still highly susceptible to H1N1 virus. However, pretreatment of D2-Mx1(r/r) mice with alpha interferon protected them from lethal infections. Our results showed, for the first time, that the presence of an Mx1 wild-type allele from A2G as such does not fully protect mice from lethal influenza A virus infections. These observations are also highly relevant for susceptibility to influenza virus infections in humans.

IMPORTANCE

Influenza A virus represents a major health threat to humans. Seasonal influenza epidemics cause high economic loss, morbidity, and deaths each year. Genetic factors of the host strongly influence susceptibility and resistance to virus infections. The Mx1 (MX dynamin-like GTPase 1) gene has been described as a major resistance gene in mice and humans. Most inbred laboratory mouse strains are deficient in Mx1, but congenic B6-Mx1(r/r) mice that carry the wild-type Mx1 gene from the A2G mouse strain are highly resistant. Here, we show that, very unexpectedly, congenic D2-Mx1(r/r) mice carrying the wild-type Mx1 gene from the A2G strain are not fully protected against lethal influenza virus infections. These observations demonstrate that the genetic background is very important for the protective function of the Mx1 resistance gene. Our results are also highly relevant for understanding genetic susceptibility to influenza virus infections in humans.

摘要

未标记

流感病毒感染对人类健康构成严重威胁。外在和内在因素决定了流感的严重程度。MX动力蛋白样GTP酶1(Mx1)基因已被证明能使小鼠对甲型流感病毒感染产生强大抗性。大多数实验室小鼠品系,包括C57BL/6J,在Mx1基因中携带无义或缺失突变,因此是无功能等位基因,而野生来源的小鼠品系携带野生型Mx1等位基因。表达来自A2G小鼠品系野生型等位基因的同基因C57BL/6J(B6-Mx1(r/r))小鼠对甲型流感病毒感染具有高度抗性,对单碱性和多碱性亚型均如此。此外,在基因定位研究中,Mx1被确定为对流感病毒感染抗性的主要基因座。在此,我们研究了Mx1的保护功能是否受遗传背景影响。为此,我们培育了一个在DBA/2J背景上携带A2G野生型Mx1抗性等位基因的同基因小鼠品系(D2-Mx1(r/r))。最值得注意的是,表达功能性Mx1野生型等位基因的同基因D2-Mx1(r/r)小鼠对H1N1病毒仍然高度易感。然而,用α干扰素预处理D2-Mx1(r/r)小鼠可使其免受致命感染。我们的结果首次表明,来自A2G的Mx1野生型等位基因本身并不能完全保护小鼠免受甲型流感病毒的致命感染。这些观察结果对于人类对流感病毒感染的易感性也具有高度相关性。

重要性

甲型流感病毒对人类健康构成重大威胁。季节性流感流行每年造成高额经济损失、发病和死亡。宿主的遗传因素强烈影响对病毒感染的易感性和抗性。Mx1(MX动力蛋白样GTP酶1)基因在小鼠和人类中被描述为主要抗性基因。大多数近交系实验室小鼠品系在Mx1方面存在缺陷,但携带来自A2G小鼠品系野生型Mx1基因的同基因B6-Mx1(r/r)小鼠具有高度抗性。在此,我们非常意外地表明,携带来自A2G品系野生型Mx1基因的同基因D2-Mx1(r/r)小鼠不能完全免受致命流感病毒感染的保护。这些观察结果表明遗传背景对于Mx1抗性基因的保护功能非常重要。我们的结果对于理解人类对流感病毒感染的遗传易感性也具有高度相关性。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/5622/4577889/d64e3819aec0/zjv9990908150001.jpg

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