Role of Cdx factors in early mesodermal fate decisions

Foley, Tanya; Hess, Bradley; Savory, Joanne G.A.; Ringuette, Randy; Lohnes, David

doi:10.1242/dev.170498

Cited by 19 publications

(21 citation statements)

References 110 publications

(247 reference statements)

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“…It has been demonstrated that Cdx2 is the predominant Cdx gene expressing the AGM HE, while the expression of other Cdx genes is substantially lower ( Gao et al, 2018 ). Cdx2 deficiency caused the most significant impairment in blood production from mouse ESCs ( Wang et al, 2008 ) and Cdx1-Cdx2 compound conditional null mice failed to produce any blood at embryonic day (E)11.5 ( Foley et al, 2019 ), suggesting that among the Cdx family, Cdx2 is the most critical factor required for establishing hematopoiesis. Our finding of the direct regulation of CDX2 expression by SOX17 provides an insight into the mechanisms responsible for establishing a CDX-HOXA pathway required for the formation of definitive AGM-like HE and lympho-myeloid hematopoiesis from hPSCs.…”

Section: Discussionmentioning

confidence: 99%

SOX17 integrates HOXA and arterial programs in hemogenic endothelium to drive definitive lympho-myeloid hematopoiesis

et al. 2021

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SUMMARY SOX17 has been implicated in arterial specification and the maintenance of hematopoietic stem cells (HSCs) in the murine embryo. However, knowledge about molecular pathways and stage-specific effects of SOX17 in humans remains limited. Here, using SOX17-knockout and SOX17-inducible human pluripotent stem cells (hPSCs), paired with molecular profiling studies, we reveal that SOX17 is a master regulator of HOXA and arterial programs in hemogenic endothelium (HE) and is required for the specification of HE with robust lympho-myeloid potential and DLL4 + CXCR4 + phenotype resembling arterial HE at the sites of HSC emergence. Along with the activation of NOTCH signaling, SOX17 directly activates CDX2 expression, leading to the upregulation of the HOXA cluster genes. Since deficiencies in HOXA and NOTCH signaling contribute to the impaired in vivo engraftment of hPSC-derived hematopoietic cells, the identification of SOX17 as a key regulator linking arterial and HOXA programs in HE may help to program HSC fate from hPSCs.

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Section: Discussionmentioning

confidence: 99%

SOX17 integrates HOXA and arterial programs in hemogenic endothelium to drive definitive lympho-myeloid hematopoiesis

et al. 2021

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“…Similarly, in mice, ectopic Tbx5 expression was observed in the yolk sac of Cdx1/2 compound conditional null mutants at the expense of hematopoietic markers [123]. Current evidence supports a mechanism of action for Cdx genes in which they stably repress cardiac loci in early Mesp1+ mesoderm by directly recruiting the SWI/SNF epigenetic silencing complex [123]. Thus, the expression of Cdx biases these progenitors to hematopoietic lineages at the expense of cardiac lineages.…”

Section: Leukemiamentioning

confidence: 95%

“…In zebrafish, the tbx5a -expressing anterior cardiogenic mesoderm was expanded in cdx1a/4 mutants [122]. Similarly, in mice, ectopic Tbx5 expression was observed in the yolk sac of Cdx1/2 compound conditional null mutants at the expense of hematopoietic markers [123]. Current evidence supports a mechanism of action for Cdx genes in which they stably repress cardiac loci in early Mesp1+ mesoderm by directly recruiting the SWI/SNF epigenetic silencing complex [123].…”

Section: Leukemiamentioning

confidence: 99%

Cdx2 Animal Models Reveal Developmental Origins of Cancers

Chawengsaksophak

2019

Genes

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The Cdx2 homeobox gene is important in assigning positional identity during the finely orchestrated process of embryogenesis. In adults, regenerative responses to tissues damage can require a replay of these same developmental pathways. Errors in reassigning positional identity during regeneration can cause metaplasias—normal tissue arising in an abnormal location—and this in turn, is a well-recognized cancer risk factor. In animal models, a gain of Cdx2 function can elicit a posterior shift in tissue identity, modeling intestinal-type metaplasias of the esophagus (Barrett’s esophagus) and stomach. Conversely, loss of Cdx2 function can elicit an anterior shift in tissue identity, inducing serrated-type lesions expressing gastric markers in the colon. These metaplasias are major risk factors for the later development of esophageal, stomach and colon cancer. Leukemia, another cancer in which Cdx2 is ectopically expressed, may have mechanistic parallels with epithelial cancers in terms of stress-induced reprogramming. This review will address how animal models have refined our understanding of the role of Cdx2 in these common human cancers.

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“…5). VIA consistently uncovers the bifurcating lineages using both single-cell transcriptomic (scRNA-seq) and chromatin accessibility (scATAC-seq) information [26][27][28] , as well as their data integration (see "Methods" for data integration using Seurat). Other methods that are also applicable to non-transcriptomic data, fail to uncover the two main lineages.…”

Section: Cd79bmentioning

confidence: 99%

“…Although PCA is a common step in analyzing transcriptomic data in order to strengthen the signal in the data, we also show that in-principle, VIA can handle 1000 s of genes as direct inputs without any PCA at all (Supplementary Note 5 and Figs. [27][28][29]. We showcase the scalability of sample size by analyzing the fine-grained developmental sub-trajectories in the 1.3million-cell mouse organogenesis atlas in terms of fast runtime and preservation of global cell-type connectivity, which is otherwise lost in existing TI methods.…”

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confidence: 99%

Generalized and scalable trajectory inference in single-cell omics data with VIA

et al. 2021

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Inferring cellular trajectories using a variety of omic data is a critical task in single-cell data science. However, accurate prediction of cell fates, and thereby biologically meaningful discovery, is challenged by the sheer size of single-cell data, the diversity of omic data types, and the complexity of their topologies. We present VIA, a scalable trajectory inference algorithm that overcomes these limitations by using lazy-teleporting random walks to accurately reconstruct complex cellular trajectories beyond tree-like pathways (e.g., cyclic or disconnected structures). We show that VIA robustly and efficiently unravels the fine-grained sub-trajectories in a 1.3-million-cell transcriptomic mouse atlas without losing the global connectivity at such a high cell count. We further apply VIA to discovering elusive lineages and less populous cell fates missed by other methods across a variety of data types, including single-cell proteomic, epigenomic, multi-omics datasets, and a new in-house single-cell morphological dataset.

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Role of Cdx factors in early mesodermal fate decisions

Cited by 19 publications

References 110 publications

SOX17 integrates HOXA and arterial programs in hemogenic endothelium to drive definitive lympho-myeloid hematopoiesis

SOX17 integrates HOXA and arterial programs in hemogenic endothelium to drive definitive lympho-myeloid hematopoiesis

Cdx2 Animal Models Reveal Developmental Origins of Cancers

Generalized and scalable trajectory inference in single-cell omics data with VIA

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