Thymic Activity and T Cell Repertoire Recovery after Autologous Hematopoietic Stem Cell Transplantation Preceded by Myeloablative Radiotherapy or Chemotherapy

Głowala-Kosińska, Magdalena; Chwieduk, Agata; Smagur, Andrzej; Fidyk, Wojciech; Najda, Jacek; Mitrus, Iwona; Giebel, Sebastian

doi:10.1016/j.bbmt.2016.01.014

Cited by 15 publications

(12 citation statements)

References 33 publications

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“…A non-significant increase in CD4 T-cell RTE and CM subset frequencies was observed in the PP women compared to PnP participants, indicating pregnancy may promote T-cell production and differentiation, while group frequencies of Ni, Tscm, EM, and Temra CD4 T-cell subsets were similar. We differentiated RTE from Ni T cells using CD31 expression and the frequencies we observed are similar to those of other recent studies exploring the RTE compartment (44)(45)(46)(47).…”

Section: No Significant Cross-sectional Difference Observed Between Tsupporting

confidence: 75%

Pregnancy Gestation Impacts on HIV-1-Specific Granzyme B Response and Central Memory CD4 T Cells

et al. 2020

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Pregnancy induces alterations in peripheral T-cell populations with both changes in subset frequencies and anti-viral responses found to alter with gestation. In HIV-1 positive women anti-HIV-1 responses are associated with transmission risk, however detailed investigation into both HIV-1-specific memory responses associated with HIV-1 control and T-cell subset changes during pregnancy have not been undertaken. In this study we aimed to define pregnancy and gestation related changes to HIV-1-specific responses and T-cell phenotype in ART treated HIV-1 positive pregnant women. Eleven non-pregnant and 24 pregnant HIV-1 positive women were recruited, peripheral blood samples taken, fresh cells isolated, and compared using ELISpot assays and flow cytometry analysis. Clinical data were collected as part of standard care, and non-parametric statistics used. Alterations in induced IFNγ, IL-2, IL-10, and granzyme B secretion by peripheral blood mononuclear cells in response to HIV-1 Gag and Nef peptide pools and changes in T-cell subsets between pregnant and non-pregnant women were assessed, with data correlated with participant clinical parameters and longitudinal analysis performed. Cross-sectional comparison identified decreased IL-10 Nef response in HIV-1 positive pregnant women compared to non-pregnant, while correlations exhibited reversed Gag and Nef cytokine and protease response associations between groups. Longitudinal analysis of pregnant participants demonstrated transient increases in Gag granzyme B response and in the central memory CD4 T-cell subset frequency during their second trimester, with a decrease in CD4 effector memory T cells from their second to third trimester. Gag and Nef HIV-1-specific responses diverge with pregnancy time-point, coinciding with relevant T-cell phenotype, and gestation associated immunological adaptations. Decreased IL-10 Nef and both increased granzyme B Gag response and central memory CD4 T cells implies that amplified antigen production is occurring, which suggests a period of compromised HIV-1 control in pregnancy.

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Section: No Significant Cross-sectional Difference Observed Between Tsupporting

confidence: 75%

Pregnancy Gestation Impacts on HIV-1-Specific Granzyme B Response and Central Memory CD4 T Cells

et al. 2020

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“…). This could result from a thymic damage caused by TBI, which may affect mainly children, who have been shown to have a lesser peripheral T‐cell expansion compared with adults . The results of the study by Sullivan et al.…”

Section: Discussionmentioning

confidence: 99%

The role of immunoglobulin prophylaxis for prevention of cytomegalovirus infection in pediatric hematopoietic stem cell transplantation recipients

Gal

Rutenberg

Mendelovich

et al. 2017

Pediatr Blood Cancer

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“…The following phenotypes were examined in CD3+ T gate: naïve T cells (Tn) CD45RA+CD62L+, central memory T cells (Tcm) CD45RA−CD62L+ and effector memory T cells (Tem) CD45RA−CD62L− within the CD3+CD4+ and CD3+CD8+ T-cell subsets; and effector memory CD45RA (TemRA) CD3+CD8+CD45RA+CD62L− T cells. In addition, the expression of CD31 was measured in Tn gates to assess the level of recent emigrants 15. All the stainings were combined with tetramer and intracellular FoxP3 stainings to assess the levels of antigen-specific CD4+FoxP3− Tconvs, CD4+FoxP3+ Tregs and CD8+ T cells.…”

Section: Methodsmentioning

confidence: 99%

Proinsulin-specific T regulatory cells may control immune responses in type 1 diabetes: implications for adoptive therapy

Gliwiński

Iwaszkiewicz-Grześ

Wołoszyn-Durkiewicz

et al. 2020

BMJ Open Diab Res Care

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ObjectiveHere we looked for possible mechanisms regulating the progression of type 1 diabetes mellitus (T1DM). In this disease, autoaggressive T cells (T conventional cells, Tconvs) not properly controlled by T regulatory cells (Tregs) destroy pancreatic islets.Research design and methodsWe compared the T-cell compartment of patients with newly diagnosed T1DM (NDT1DM) with long-duration T1DM (LDT1DM) ones. The third group consisted of patients with LDT1DM treated previously with polyclonal Tregs (LDT1DM with Tregs). We have also looked if the differences might be dependent on the antigen specificity of Tregs expanded for clinical use and autologous sentinel Tconvs.ResultsPatients with LDT1DM were characterized by T-cell immunosenescence-like changes and expansion of similar vβ/T-cell receptor (TCR) clones in Tconvs and Tregs. The treatment with Tregs was associated with some inhibition of these effects. Patients with LDT1DM possessed an increased percentage of various proinsulin-specific T cells but not GAD65-specific ones. The percentages of all antigen-specific subsets were higher in the expansion cultures than in the peripheral blood. The proliferation was more intense in proinsulin-specific Tconvs than in specific Tregs but the levels of some proinsulin-specific Tregs were exceptionally high at baseline and remained higher in the expanded clinical product than the levels of respective Tconvs in sentinel cultures.ConclusionsT1DM is associated with immunosenescence-like changes and reduced diversity of T-cell clones. Preferential expansion of the same TCR families in both Tconvs and Tregs suggests a common trigger/autoantigen responsible. Interestingly, the therapy with polyclonal Tregs was associated with some inhibition of these effects. Proinsulin-specific Tregs appeared to be dominant in the immune responses in patients with T1DM and probably associated with better control over respective autoimmune Tconvs.Trial registration numberEudraCT 2014-004319-35.

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Thymic Activity and T Cell Repertoire Recovery after Autologous Hematopoietic Stem Cell Transplantation Preceded by Myeloablative Radiotherapy or Chemotherapy

Cited by 15 publications

References 33 publications

Pregnancy Gestation Impacts on HIV-1-Specific Granzyme B Response and Central Memory CD4 T Cells

Pregnancy Gestation Impacts on HIV-1-Specific Granzyme B Response and Central Memory CD4 T Cells

The role of immunoglobulin prophylaxis for prevention of cytomegalovirus infection in pediatric hematopoietic stem cell transplantation recipients

Proinsulin-specific T regulatory cells may control immune responses in type 1 diabetes: implications for adoptive therapy

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