Axial skeleton anterior-posterior patterning is regulated through feedback regulation between Meis transcription factors and retinoic acid

López-Delgado, Alejandra Cristina; Delgado, Irene; Cadenas, Vanessa; Sánchez-Cabo, Fátima; Torres, Miguel

doi:10.1242/dev.193813

Cited by 11 publications

(7 citation statements)

References 79 publications

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“…The first COVET DC reveals that scRNA-seq cells are correctly enriched for Hoxd4 48,52 (anterior) and Hoxb9 53 (posterior) markers in their respective domains, consistent with seqFISH expression in NMP and spine cells (Fig. 5c).…”

Section: Envi Learns Spatial Gradients From Single-cell Datasupporting

confidence: 71%

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The covariance environment defines cellular niches for spatial inference

Haviv

Gatie

Hadjantonakis

et al. 2023

Preprint

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The tsunami of new multiplexed spatial profiling technologies has opened a range of computational challenges focused on leveraging these powerful data for biological discovery. A key challenge underlying computation is a suitable representation for features of cellular niches. Here, we develop the covariance environment (COVET), a representation that can capture the rich, continuous multivariate nature of cellular niches by capturing the gene-gene covariate structure across cells in the niche, which can reflect the cell-cell communication between them. We define a principled optimal transport-based distance metric between COVET niches and develop a computationally efficient approximation to this metric that can scale to millions of cells. Using COVET to encode spatial context, we develop environmental variational inference (ENVI), a conditional variational autoencoder that jointly embeds spatial and single-cell RNA-seq data into a latent space. Two distinct decoders either impute gene expression across spatial modality, or project spatial information onto dissociated single-cell data. We show that ENVI is not only superior in the imputation of gene expression but is also able to infer spatial context to disassociated single-cell genomics data.

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Section: Envi Learns Spatial Gradients From Single-cell Datasupporting

confidence: 71%

“…Hoxb7 and Tlx2 78 ) and anterior genes (Foxa3 79,80 , Hoxd3 52 , Hoxa2 [81][82][83] , Rfx4 and Hoxd4).…”

Section: Mapping Cortical Depth Of Dissociated Neurons With Merfishunclassified

The covariance environment defines cellular niches for spatial inference

Haviv

Gatie

Hadjantonakis

et al. 2023

Preprint

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“…Indeed, putative enhancer regions identified in pSHF cells revealed enrichment for HOX and TALE binding motifs (Stefanovic et al, 2020). While HOX and MEIS genes appear to be direct targets of RA itself (Mercader et al, 2000;Berenguer et al, 2020), studies have shown that they can also regulate Raldh2 expression and thereby RA levels through a positive feedback loop (Vitobello et al, 2011;Lo ´pez-Delgado et al, 2021). Interestingly, misexpression of Hoxb1 in the aSHF domain resulted in an upregulation of Tbx5 and Nr2f2 (Stefanovic et al, 2020), both of which are implicated in the differentiation of atrial and sinoatrial nodal cells in vivo and in vitro (Liberatore et al, 2000;Wu et al, 2013;Devalla et al, 2015;Protze et al, 2017).…”

Section: Stem Cell Reportsmentioning

confidence: 99%

Retinoic acid signaling in heart development: Application in the differentiation of cardiovascular lineages from human pluripotent stem cells

et al. 2021

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Retinoic acid (RA) signaling plays an important role during heart development in establishing anteroposterior polarity, formation of inflow and outflow tract progenitors, and growth of the ventricular compact wall. RA is also utilized as a key ingredient in protocols designed for generating cardiac cell types from pluripotent stem cells (PSCs). This review discusses the role of RA in cardiogenesis, currently available protocols that employ RA for differentiation of various cardiovascular lineages, and plausible transcriptional mechanisms underlying this fate specification. These insights will inform further development of desired cardiac cell types from human PSCs and their application in preclinical and clinical research.

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“…During embryo development, Meis1 ablation results in hematopoietic, vascular, and ocular defects [2,3]. It has been also well defined the role of Meis1 and Meis2 in mouse axial skeleton formation [7][8][9] and in anterior-posterior patterning for limb initiation [10], for which Meis loss-of-function (Meis1 and Meis2 double knock-out) embryos are limbless, with undeveloped appendicular condensations.…”

Section: Introductionmentioning

confidence: 99%

MEIS1 in Hematopoiesis and Cancer. How MEIS1-PBX Interaction Can Be Used in Therapy

Blasi

Bruckmann

2021

JDB

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Recently MEIS1 emerged as a major determinant of the MLL-r leukemic phenotype. The latest and most efficient drugs effectively decrease the levels of MEIS1 in cancer cells. Together with an overview of the latest drugs developed to target MEIS1 in MLL-r leukemia, we review, in detail, the role of MEIS1 in embryonic and adult hematopoiesis and suggest how a more profound knowledge of MEIS1 biochemistry can be used to design potent and effective drugs against MLL-r leukemia. In addition, we present data showing that the interaction between MEIS1 and PBX1 can be blocked efficiently and might represent a new avenue in anti-MLL-r and anti-leukemic therapy.

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Axial skeleton anterior-posterior patterning is regulated through feedback regulation between Meis transcription factors and retinoic acid

Cited by 11 publications

References 79 publications

The covariance environment defines cellular niches for spatial inference

The covariance environment defines cellular niches for spatial inference

Retinoic acid signaling in heart development: Application in the differentiation of cardiovascular lineages from human pluripotent stem cells

MEIS1 in Hematopoiesis and Cancer. How MEIS1-PBX Interaction Can Be Used in Therapy

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