Philippe Moreau scite author profile

The HLA-G gene displays several peculiarities that are distinct from those of classical HLA class I genes. The unique structure of the HLA-G molecule permits a restricted peptide presentation and allows the modulation of the cells of the immune system. Although polymorphic sites may potentially influence all biological functions of HLA-G, those present at the promoter and 3′ untranslated regions have been particularly studied in experimental and pathological conditions. The relatively low polymorphism observed in the MHC-G coding region both in humans and apes may represent a strong selective pressure for invariance, whereas, in regulatory regions several lines of evidence support the role of balancing selection. Since HLA-G has immunomodulatory properties, the understanding of gene regulation and the role of polymorphic sites on gene function may permit an individualized approach for the future use of HLA-G for therapeutic purposes.

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HLA-G: from biology to clinical benefits

Carosella¹,

Moreau²,

LeMaoult³

et al. 2008

Trends in Immunology

333

360

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The 14 bp Deletion-Insertion polymorphism in the 3′ UT region of the HLA-G gene influences HLA-G mRNA stability

et al. 2003

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Beyond the increasing complexity of the immunomodulatory HLA-G molecule

et al. 2008

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Philippe Moreau

Implications of the polymorphism of HLA-G on its function, regulation, evolution and disease association

HLA-G: from biology to clinical benefits

The 14 bp Deletion-Insertion polymorphism in the 3′ UT region of the HLA-G gene influences HLA-G mRNA stability

Beyond the increasing complexity of the immunomodulatory HLA-G molecule

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