RBPJ-dependent Notch signaling initiates the T cell program in a subset of thymus-seeding progenitors

Chen, Edward L. Y.; Thompson, Patrycja K.; Zúñiga‐Pflücker, Juan Carlos

doi:10.1038/s41590-019-0518-7

Cited by 70 publications

(69 citation statements)

References 62 publications

(57 reference statements)

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“…Also their topology within the thymus suggests that these TSP1s represent the canonical T cell precursors that differentiate into ETPs when they encounter Notch activating signals within the thymic microenvironment. And while TSP1s themselves do not display any signs of Notch activation, we also identified a lin -CD34 + CD44 hi CD7 int CD10seeding population which resembles the Notch-primed TSPs that have been described in the BM of mice (Chen et al, 2019;Yu et al, 2015) . This TSP2 population indeed expresses the Notch target genes CD7 and CD3E prior to thymic entry, consistent with these studies.…”

Section: Discussionsupporting

confidence: 54%

Single cell profiling of immature human postnatal thymocytes resolves the complexity of intra-thymic lineage differentiation and thymus seeding precursors

Lavaert

Vandamme

et al. 2020

Preprint

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During postnatal life, thymopoiesis depends on the continuous colonization of the thymus by bone marrow derived hematopoietic progenitors that migrate through the bloodstream. In human, the nature of these thymus immigrants has remained unclear. Here, we employ single-cell RNA sequencing on approximately 70.000 CD34 + thymocytes to unravel the heterogeneity of the human immature postnatal thymocytes. Integration of bone marrow and peripheral blood precursors datasets identifies several putative thymus seeding precursors that display heterogeneity for currently used surface markers as revealed by CITEseq. Besides T cell precursors, we discover branches of intrathymic developing dendritic cells with predominantly plasmacytoid DCs. Trough trajectory inference, we delineate the transcriptional dynamics underlying early human T-lineage development from which we predict transcription factor modules that drive stage-specific steps of human T cell development. Thus, our work resolves the heterogeneity of thymus seeding precursors in human and reveals the molecular mechanisms that drive their in vivo cell fate.

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Section: Discussionsupporting

confidence: 54%

Single cell profiling of immature human postnatal thymocytes resolves the complexity of intra-thymic lineage differentiation and thymus seeding precursors

Lavaert

Vandamme

et al. 2020

Preprint

View full text Add to dashboard Cite

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“…We therefore compared expression of Notch-associated DEG from DP datasets, and found increased expression of many genes upregulated by Notch signalling in the Bcl6coKO compared to control, and decreased expression of genes that are downregulated by Notch activation in thymocytes (Arenzana et al, 2015;Chen et al, 2019) ( Figure 4A). Consequently, to test on a wider set of genes if conditional deletion of Bcl6 led to an overall increase in Notch-mediated transcription, we carried out CCA to compare our DP datasets to the transcriptome of control thymocytes and those with enhanced Notch1-mediated transcription (Arenzana et al, 2015).…”

Section: Conditional Deletion Of Bcl6 Increases Notch-mediated Transcmentioning

confidence: 99%

The transcriptional repressor Bcl6 promotes pre-TCR induced differentiation to CD4+CD8+ thymocyte and attenuates Notch1 activation

et al. 2020

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Pre-TCR signal transduction is required for developing thymocytes to differentiate from CD4-CD8- double negative (DN) to CD4+CD8+ double positive (DP) cell. Notch signalling is required for T-cell fate specification and must be maintained throughout β-selection, but inappropriate Notch activation in DN4 and DP cells is oncogenic. Here, we show that pre-TCR signalling leads to increased expression of the transcriptional repressor Bcl6 and that Bcl6 is required for differentiation to DP. Conditional deletion of Bcl6 from thymocytes reduced pre-TCR-induced differentiation to DP cell, disrupted expansion and enrichment of icTCRβ+ cells within the DN population and increased DN4 cell death. It also increased Notch1 activation and Notch-mediated transcription in the DP population. Thus, Bcl6 is required in thymocyte development for efficient differentiation from DN3 to DP cell and to attenuate Notch1 activation in DP cells. Given the importance of inappropriate NOTCH1 signalling in T-ALL, and the involvement of Bcl6 in other types of leukaemia, this study is important to our understanding of T-ALL.

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“…This results increased apoptosis of TECs, dysregulated lineage-commitment checkpoints, diminished TCR repertoire and low thymic output, all of which ultimately dampen immunosurveillance and promote tumor escape. In immature DN2 T cell subsets, CCR7 is a target of Notch1 and is important for the migration of developing T cell precursors through the thymic cortex to medulla ( 102 – 104 ). Reduction in expression levels of Notch1 and its targets in thymic pre-T cells of tumor-bearing mice is mediated by IL-10 produced by thymic epithelial cells (TECs) ( 45 ).…”

Section: Restoring Dll1-specific Notch Signaling Can Reverse Impairedmentioning

confidence: 99%

Specific Targeting of Notch Ligand-Receptor Interactions to Modulate Immune Responses: A Review of Clinical and Preclinical Findings

et al. 2020

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Understanding and targeting Notch signaling effectively has long been valued in the field of cancer and other immune disorders. Here, we discuss key discoveries at the intersection of Notch signaling, cancer and immunology. While there is a plethora of Notch targeting agents tested in vitro, in vivo and in clinic, undesirable off-target effects and therapy-related toxicities have been significant obstacles. We make a case for the clinical application of ligand-derived and affinity modifying compounds as novel therapeutic agents and discuss major research findings with an emphasis on Notch ligand-specific modulation of immune responses.

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RBPJ-dependent Notch signaling initiates the T cell program in a subset of thymus-seeding progenitors

Cited by 70 publications

References 62 publications

Single cell profiling of immature human postnatal thymocytes resolves the complexity of intra-thymic lineage differentiation and thymus seeding precursors

Single cell profiling of immature human postnatal thymocytes resolves the complexity of intra-thymic lineage differentiation and thymus seeding precursors

The transcriptional repressor Bcl6 promotes pre-TCR induced differentiation to CD4+CD8+ thymocyte and attenuates Notch1 activation

Specific Targeting of Notch Ligand-Receptor Interactions to Modulate Immune Responses: A Review of Clinical and Preclinical Findings

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