2016
DOI: 10.1016/j.jaci.2015.08.022
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Identification of checkpoints in human T-cell development using severe combined immunodeficiency stem cells

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Cited by 28 publications
(35 citation statements)
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“…For the other types of SCID, using confirmed null mutants, we observed a complete lack of peripheral T cells, which could be attributed to a severe, early, and complete block in thymic development. 78 The arrests in T cell development observed for the different types of SCID demonstrate a hierarchy in TCR rearrangement and the corresponding phenotypes (Fig. 3).…”
Section: Human Scid As a System To Understand Functional Requirementsmentioning
confidence: 93%
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“…For the other types of SCID, using confirmed null mutants, we observed a complete lack of peripheral T cells, which could be attributed to a severe, early, and complete block in thymic development. 78 The arrests in T cell development observed for the different types of SCID demonstrate a hierarchy in TCR rearrangement and the corresponding phenotypes (Fig. 3).…”
Section: Human Scid As a System To Understand Functional Requirementsmentioning
confidence: 93%
“…TCR rearrangements were functionally required at the CD4 -CD8 -CD7 + CD5 + stage, given the developmental block and extent of rearrangements in mice transplanted with Artemis-SCID. 78 The blocks in development, occurring in the immature DN stages, are much earlier than previously assumed on the basis of mouse data 80 or gene expression profiling. 5 They indicate that human ␤ selection may occur as early as the CD34 + CD1a -CD7 + CD5 + stage.…”
Section: Human Scid As a System To Understand Functional Requirementsmentioning
confidence: 96%
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“…X-SCID is caused by mutations in the gene encoding the g common chain shared by several cytokine receptors, including the interleukin (IL)-2, IL-4, IL-7, IL-9, IL-15, and IL-21 receptors. In view of these receptors' roles in hematopoiesis, X-SCID is characterized by an early block in T and NK cell differentiation, the complete absence of T and NK cells and normal-to-elevated numbers of poorly functional, mature B cells [12,13].…”
Section: Severe Combined Immunodeficienciesmentioning
confidence: 99%
“…Studies on primary immunodeficiency (61, 62), and on the immunological reconstitution achieved by the appropriate correction of these defects with HSCT (63), gene therapy (6466), or thymus transplantation (67, 68), have been instrumental to better understand T-cell development. As an illustrative example of the knowledge that can be gathered from these clinical cases, we showed that the activity of thymus explants, evaluated by sj/βTREC ratio, drastically diminished 3 years post-thymic transplantation in a case of athymia due to FOXN1 deficiency (68).…”
Section: Establishment Of the Naïve Cd4+ T-cell Compartmentmentioning
confidence: 99%