2012
DOI: 10.1038/bmt.2012.174
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Stem cell source-dependent reconstitution of FOXP3+ T cells after pediatric SCT and the association with allo-reactive disease

Abstract: In adult patients, regulatory CD4 þ FOXP3 þ T cells are suggested to have a role in the control of allo-reactive disease after hematopoietic SCT (HSCT). We compared CD4 þ FOXP3 þ T-cell reconstitution after unrelated cord blood (UCB), matched unrelated donor (MUD) and matched sibling donor (MSD) HSCT in children, starting as early as 1 week after transplantation, and analyzed the association with allo-reactive disease. A total of 30 children were included who underwent a myeloablative-conditioning regimen foll… Show more

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Cited by 5 publications
(10 citation statements)
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“…They are critical in controlling responses from other immune cell subsets to self and foreign antigens, and play a central role in preventing autoimmune disease. Tregs can be subdivided into naturally occurring Tregs, derived from the thymus, and induced Tregs, which are differentiated from nonregulatory CD4 + CD25 + cells [1,57]. Induced Tregs are more susceptible to apoptosis and have a less stable expression of FoxP3 [57].…”
Section: Tregsmentioning
confidence: 99%
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“…They are critical in controlling responses from other immune cell subsets to self and foreign antigens, and play a central role in preventing autoimmune disease. Tregs can be subdivided into naturally occurring Tregs, derived from the thymus, and induced Tregs, which are differentiated from nonregulatory CD4 + CD25 + cells [1,57]. Induced Tregs are more susceptible to apoptosis and have a less stable expression of FoxP3 [57].…”
Section: Tregsmentioning
confidence: 99%
“…Reconstitution of Tregs has been suggested to be primarily achieved by HPE without major contribution of thymopoiesis, especially compared to reconstitution of effector T cells [18,51,62,65]. The proportion of Tregs among the CD4 + T cell population returns to normal within 6 weeks post-HCT, as soon as the CD4 + T cells are detectable [57,60]. In the subsequent 2 to 3 months, differences in the stability of this proportion have been observed [57,60], which might be related to a higher proportion of activation-induced Tregs, the occurrence of GvHD (and associated treatment) and thymopoiesis.…”
Section: Tregsmentioning
confidence: 99%
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“…A limited number of studies described reconstitution of FoxP3 þ Tregs after UCBT and BMT, which takes 1 to 6 weeks for both sources, even with ATG in the conditioning [20,30] (Table 2). When comparing UCB, sibling BM, and unrelated BM transplantations, Treg reconstitution after UCBT and sibling BMT is much faster than after unrelated BMT [30]. The results in UCBT may be associated with the finding that fetal T cells more easily develop into Tregs than adult T cells [67].…”
Section: Tregmentioning
confidence: 99%
“…The negative selection relies on the ectopic expression of tissue-restricted peripheral self-antigens (TRA) in mature medullary thymic epithelial cells, which may be damaged in patients with impaired thymic function, thus, lead to compromised negative selection and GVHD [27,29]. Moreover, another mechanism relevant to thymic function could implicate donor-derived CD4 CD25high regulatory T (Treg)-cell reconstitution [30,31]. Those cells were also selected in the thymus, a competent thymic is needed for regulatory T-cells recovery in AHSCT patients [32].…”
Section: Discussionmentioning
confidence: 99%