Diez-Fuertes Francisco, López-Huertas María Rosa, García-Pérez Javier, Calonge Esther, Bermejo Mercedes, Mateos Elena, Martí Pilar, Muelas Nuria, Vílchez Juan Jesús, Coiras Mayte, Alcamí José, Rodríguez-Mora Sara
AIDS Immunopathogenesis Unit, National Center of Microbiology, Instituto de Salud Carlos III, Madrid, Spain.
Centro de Investigación Biomédica en Red de Enfermedades Infecciosas (CIBERINFEC), Madrid, Spain.
Front Cell Dev Biol. 2022 May 13;10:839813. doi: 10.3389/fcell.2022.839813. eCollection 2022.
LGMDD2 is a rare form of muscular dystrophy characterized by one of the three heterozygous deletions described within the gene that result in the addition of a 15-amino acid tail in the C-terminus.TNPO3 is involved in the nuclear import of splicing factors and acts as a host cofactor for HIV-1 infection by mechanisms not yet deciphered. Further characterization of the crosstalk between HIV-1 infection and LGMDD2 disease may contribute to a better understanding of both the cellular alterations occurring in LGMDD2 patients and the role of TNPO3 in the HIV-1 cycle. To this regard, transcriptome profiling of PBMCs from LGMDD2 patients carrying the deletion c.2771delA in the gene was compared to healthy controls. A total of 545 differentially expressed genes were detected between LGMDD2 patients and healthy controls, with a high representation of G protein-coupled receptor binding chemokines and metallopeptidases among the most upregulated genes in LGMDD2 patients. Plasma levels of IFN-β and IFN-γ were 4.7- and 2.7-fold higher in LGMDD2 patients, respectively. An increase of 2.3-fold in the expression of the interferon-stimulated gene MxA was observed in activated PBMCs from LGMDD2 patients after HIV-1 pseudovirus infection. Thus, the analysis suggests a pro-inflammatory state in LGMDD2 patients also described for other muscular dystrophies, that is characterized by the alteration of IL-17 signaling pathway and the consequent increase of metallopeptidases activity and TNF response. In summary, the increase in interferons and inflammatory mediators suggests an antiviral environment and resistance to HIV-1 infection but that could also impair muscular function in LGMDD2 patients, worsening disease evolution. Biomarkers of disease progression and therapeutic strategies based on these genes and mechanisms should be further investigated for this type of muscular dystrophy.
LGMDD2是一种罕见的肌肉萎缩症,其特征是该基因内描述的三种杂合缺失之一,导致C末端添加了一个15个氨基酸的尾巴。TNPO3参与剪接因子的核输入,并通过尚未阐明的机制作为HIV-1感染的宿主辅助因子。进一步表征HIV-1感染与LGMDD2疾病之间的相互作用,可能有助于更好地理解LGMDD2患者发生的细胞改变以及TNPO3在HIV-1周期中的作用。在这方面,将携带该基因c.2771delA缺失的LGMDD2患者的外周血单核细胞(PBMC)转录组谱与健康对照进行了比较。在LGMDD2患者和健康对照之间共检测到545个差异表达基因,其中G蛋白偶联受体结合趋化因子和金属肽酶在LGMDD2患者中上调最多的基因中占很高比例。LGMDD2患者血浆中IFN-β和IFN-γ水平分别高出4.7倍和2.7倍。在HIV-1假病毒感染后,LGMDD2患者活化的PBMC中干扰素刺激基因MxA的表达增加了2.3倍。因此,该分析表明LGMDD2患者存在促炎状态,其他肌肉萎缩症也有描述,其特征是IL-17信号通路改变,随之金属肽酶活性和TNF反应增加。总之,干扰素和炎症介质的增加表明存在抗病毒环境以及对HIV-1感染的抗性,但这也可能损害LGMDD2患者的肌肉功能,使疾病进展恶化。对于这种类型的肌肉萎缩症,应进一步研究基于这些基因和机制的疾病进展生物标志物和治疗策略。
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