Kerri Packwood scite author profile

Summary Common variable immunodeficiency disorders (CVID) are a group of heterogeneous conditions that have in common primary failure of B cell function, although numerous T cell abnormalities have been described, including reduced proliferative response and reduced regulatory T cells. This study compared the T cell phenotype of CVID patients subdivided into clinical phenotypes as well as patients with partial antibody deficiencies [immunoglobulin (Ig)G subclass deficiency and selective IgA deficiency], X‐linked agammaglobulinaemia (XLA) and healthy and disease controls. Absolute numbers of T cell subpopulations were measured by four‐colour flow cytometry: naive T cells, central and effector memory and terminally differentiated (TEM) T cells, using CD45RA and CCR7 expression. Early, intermediate and late differentiation status of T cells was measured by CD27/CD28 expression. Putative follicular T cells, recent thymic emigrants and regulatory T cells were also assessed. Significant reduction in naive CD4 T cells, with reduced total CD4 and recent thymic emigrant numbers, was observed in CVID patients, most pronounced in those with autoimmune cytopenias or polyclonal lymphoproliferation. These findings suggest a lack of replenishment by new thymically derived cells. CD8 naive T cells were reduced in CVID patients, most significantly in the autoimmune cytopenia subgroup. There was a reduction in early differentiated CD4 and CD8 T cells and increased CD8 TEM in the CVID patients, particularly autoimmune cytopenia and polyclonal lymphoproliferation subgroups, suggesting a more activated T cell phenotype, due perhaps to an antigen‐driven process. XLA patients had significantly reduced putative follicular T cells, which may depend on B cells for survival, while no significant alterations were observed in the T cells of those with IgG subclass deficiency or selective IgA deficiency.

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A pharmacokinetic analysis of posaconazole oral suspension in the serum and alveolar compartment of lung transplant recipients

Thakuria

Packwood

Firouzi

et al. 2016

International Journal of Antimicrobial Agents

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NOD2polymorphisms in clinical phenotypes of common variable immunodeficiency disorders

Packwood¹,

Drewe

Staples

et al. 2010

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SummaryCommon variable immunodeficiency disorders (CVIDs) are a heterogeneous group of diseases characterized by hypogammaglobulinaemia and consequent susceptibility to infection. CVID patients commonly develop a variety of additional manifestations for which the causative factors are not fully understood. Two such manifestations are granulomatous disease and enteropathy. Because the ability to predict complications would aid clinical management, we continue to search for possible disease modifier genes. NOD2 acts a microbial sensor and is involved in proinflammatory signalling. Particular mutations of the NOD2 gene are associated with Crohn's disease including gly908arg, leu1007finsc and arg702trp polymorphisms. We hypothesized that NOD2 polymorphisms may be a disease modifier gene towards an enteropathic or granulomatous phenotype within CVIDs. Sequence-specific primers returned genotypes for 285 CVID patients from centres across the United Kingdom and Europe. We present the frequencies of the different phenotypes of patients within our international cohort. Arg702trp polymorphisms were significantly less frequent than wild-type (WT) (P = 0·038) among international CVID patients with splenomegaly. Gly908arg polymorphisms were more prevalent than WT in UK patients with autoimmune disorders (P = 0·049) or enteropathy (P = 0·049). NOD2 polymorphisms were not more prevalent than WT in CVID patients with clinical phenotypes of granulomata. UK allele frequencies of 0·014, 0·056 and 0·026 were found for gly908arg, arg702trp and leu1007finsc NOD2 polymorphisms, respectively. These do not differ significantly from UK immunocompetent controls confirming, as expected, that in addition these NOD2 polymorphisms do not confer susceptibility to CVIDs per se.

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F.77. Can the Frequency of Memory B Cells be Used to Diagnose Primary Antibody Failure?

Bateman¹,

Lucas²,

Packwood³

et al. 2008

Clinical Immunology

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Introduction to Proteomics, Principles and Applications Navin C. Mishra Foreword by Guenter Blobel John Wiley and Sons, 2010, pp. 200 Print ISBN: 978‐0471754022 Online ISBN: 978‐0470603871

Packwood

2011

Proteomics

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NOD2 Polymorphisms in CVID: Investigation into Associations with Gastrointestinal Pathology and Granulomatous Disease

Packwood¹,

Ferry²,

Punwani³

et al. 2007

Clinical Immunology

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Kerri Packwood

T cell phenotypes in patients with common variable immunodeficiency disorders: associations with clinical phenotypes in comparison with other groups with recurrent infections

A pharmacokinetic analysis of posaconazole oral suspension in the serum and alveolar compartment of lung transplant recipients

NOD2polymorphisms in clinical phenotypes of common variable immunodeficiency disorders

F.77. Can the Frequency of Memory B Cells be Used to Diagnose Primary Antibody Failure?

Introduction to Proteomics, Principles and Applications Navin C. Mishra Foreword by Guenter Blobel John Wiley and Sons, 2010, pp. 200 Print ISBN: 978‐0471754022 Online ISBN: 978‐0470603871

NOD2 Polymorphisms in CVID: Investigation into Associations with Gastrointestinal Pathology and Granulomatous Disease

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