Khaleel Jamil scite author profile

The innate immune system is the first line of defence in response to pathogen infection. Natural killer (NK) cells perform a vital role in this response with the ability to directly kill infected cells, produce cytokines, and cross-talk with the adaptive immune system. These effector functions are dependent on activation of NK cells which is determined by surface receptor interactions with ligands on target cells. Of these receptors, the polymorphic killer immunoglobulin-like receptors (KIRs), which interact with MHC class 1 (also highly polymorphic), are largely inhibitory, and exhibit substantial genetic diversity. The result is a significant variation of NK cell repertoire between individuals and also between populations, with a multitude of possible KIR:HLA combinations. As each KIR:ligand interaction may have differential effects on NK cell activation and inhibition, this diversity has important potential influences on the host response to infections. Genetic studies have demonstrated associations between specific KIR:ligand combinations and the outcome of viral (and other) infections, in particular hepatitis C and HIV infection. Detailed functional studies are not required to define the mechanisms underpinning these disease associations.

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The impact of organ dysfunction in cirrhosis: Survival at a cost?

Shawcross

Austin

Abeles

et al. 2012

Journal of Hepatology

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Synergistic inhibition of natural killer cells by the nonsignaling molecule CD94

Cheent

Jamil

Cassidy

et al. 2013

Proc. Natl. Acad. Sci. U.S.A.

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Peptide selectivity is a feature of inhibitory receptors for MHC class I expressed by natural killer (NK) cells. CD94-NKG2A operates in tandem with the polymorphic killer cell Ig-like receptors (KIR) and Ly49 systems to inhibit NK cells. However, the benefits of having two distinct inhibitory receptor-ligand systems are not clear. We show that noninhibitory peptides presented by HLA-E can augment the inhibition of NKG2A + NK cells mediated by MHC class I signal peptides through the engagement of CD94 without a signaling partner. Thus, CD94 is a peptide-selective NK cell receptor, and NK cells can be regulated by nonsignaling interactions. We also show that KIR + and NKG2A + NK cells respond with differing stoichiometries to MHC class I down-regulation. MHC-I-bound peptide functions as a molecular rheostat controlling NK cell function. Selected peptides which in isolation do not inhibit NK cells can have different effects on KIR and NKG2A receptors. Thus, these two inhibitory systems may complement each other by having distinct responses to bound peptide and surface levels of MHC class I.innate immunity | MHC-I peptides

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Interferon‐induced thyroid dysfunction in chronic hepatitis C

Jamil¹,

Leedman

Kontorinis³

et al. 2009

J of Gastro and Hepatol

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Khaleel Jamil

KIR/HLA Interactions and Pathogen Immunity

The impact of organ dysfunction in cirrhosis: Survival at a cost?

Synergistic inhibition of natural killer cells by the nonsignaling molecule CD94

Interferon‐induced thyroid dysfunction in chronic hepatitis C

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