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Erratum: Host non-inflammatory neutrophils mediate the engraftment of bioengineered vascular networks

Ruei-Zeng Lin
Chin Nien Lee
Juan M. Melero-Martin
Amendments and Corrections26 Jun 2017
Nature Biomedical Engineering

Volume: 1, P: 1
Author Correction: Massively parallel in vivo CRISPR screening identifies RNF20/40 as epigenetic regulators of cardiomyocyte maturation

Nathan J. VanDusen
Julianna Y. Lee
William T. Pu
Amendments and CorrectionsOpen Access19 Aug 2021
Nature Communications

Volume: 12, P: 1
Molecule in mothers’ milk nurses pups’ heart cells to maturity

A fatty acid in the milk of nursing mice has been found to trigger a transformation in the metabolic pathways that are active in pups’ heart muscle cells, enabling the cells to rapidly mature after birth.

Pingzhu Zhou
William T. Pu
News & Views24 May 2023
Nature

Volume: 618, P: 242-243
A reference map of murine cardiac transcription factor chromatin occupancy identifies dynamic and conserved enhancers

Mapping transcription factors (TFs) occupancy is essential for understanding transcriptional programs. Here the authors use biotinylated knockin alleles of key cardiac TFs (GATA4, NKX2-5, MEF2A, MEF2C, SRF, TBX5, TEAD1) to map their genome-wide occupancy in the fetal and adult mouse heart, providing insight into the cardiac transcriptional regulatory network.

Brynn N. Akerberg
Fei Gu
William T. Pu
ResearchOpen Access28 Oct 2019
Nature Communications

Volume: 10, P: 1-16
Functional dissection of human cardiac enhancers and noncoding de novo variants in congenital heart disease

Lentiviral massively parallel reporter assay (lentiMPRA) analysis of cardiac cis-regulatory elements characterizes the effects of noncoding de novo variants identified in congenital heart disease. EpiCard is a model for variant prioritization.

Feng Xiao
Xiaoran Zhang
William T. Pu
Research20 Feb 2024
Nature Genetics

Volume: 56, P: 420-430
Massively parallel in vivo CRISPR screening identifies RNF20/40 as epigenetic regulators of cardiomyocyte maturation

Throughput of in vivo genetic screens is a barrier to efficient application. Here the authors use a high-throughput CRISPR-based in vivo forward genetic screen in mice to identify transcriptional regulators of cardiomyocyte maturation, including the epigenetic modifiers RNF20 and RNF40.

Nathan J. VanDusen
Julianna Y. Lee
William T. Pu
ResearchOpen Access21 Jul 2021
Nature Communications

Volume: 12, P: 1-12
Host non-inflammatory neutrophils mediate the engraftment of bioengineered vascular networks

A comparison of the in vivo engraftment of scaffolds containing either an unassembled suspension of human vascular cells or an assembled network of them shows that non-inflammatory host neutrophils are indispensable mediators of vascularization.

Ruei-Zeng Lin
Chin Nien Lee
Juan M. Melero-Martin
Research13 Jun 2017
Nature Biomedical Engineering

Volume: 1, P: 1-13
Hierarchical and stage-specific regulation of murine cardiomyocyte maturation by serum response factor

The processes regulating cardiomyocyte (CM) maturation are unclear. Here, the authors show that serum response factor regulates CM maturation only in neonatal CMs through stage-specific chromatin occupancy that affects cell size, sarcomere and transverse-tubule organization, and mitochondria

Yuxuan Guo
Blake D. Jardin
William T. Pu
ResearchOpen Access21 Sept 2018
Nature Communications

Volume: 9, P: 1-16
VEGF amplifies transcription through ETS1 acetylation to enable angiogenesis

Promoter proximal RNAPII pausing is a rate-limiting transcriptional mechanism. Chen et al. show that this process is essential in angiogenesis by demonstrating that the endothelial master transcription factor ETS1 promotes global RNAPII pause release, and that this process is governed by VEGF.

Jiahuan Chen
Yi Fu
William T. Pu
ResearchOpen Access29 Aug 2017
Nature Communications

Volume: 8, P: 1-13
Trbp regulates heart function through microRNA-mediated Sox6 repression

Da-Zhi Wang and colleagues knock out Trbp in mouse cardiomyocytes in vivo and investigate its requirement for normal heart function. They find that Trbp is necessary for the biogenesis of miR-208a, which targets and represses Sox6.

Jian Ding
Jinghai Chen
Da-Zhi Wang
Research01 Jun 2015
Nature Genetics

Volume: 47, P: 776-783

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Erratum: Host non-inflammatory neutrophils mediate the engraftment of bioengineered vascular networks

Author Correction: Massively parallel in vivo CRISPR screening identifies RNF20/40 as epigenetic regulators of cardiomyocyte maturation

Molecule in mothers’ milk nurses pups’ heart cells to maturity

A reference map of murine cardiac transcription factor chromatin occupancy identifies dynamic and conserved enhancers

Functional dissection of human cardiac enhancers and noncoding de novo variants in congenital heart disease

Massively parallel in vivo CRISPR screening identifies RNF20/40 as epigenetic regulators of cardiomyocyte maturation

Host non-inflammatory neutrophils mediate the engraftment of bioengineered vascular networks

Hierarchical and stage-specific regulation of murine cardiomyocyte maturation by serum response factor

VEGF amplifies transcription through ETS1 acetylation to enable angiogenesis

Trbp regulates heart function through microRNA-mediated Sox6 repression

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