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Literature DB >> 24418654

Sox17 is required for normal pulmonary vascular morphogenesis.

Alexander W Lange¹, Hans Michael Haitchi², Timothy D LeCras¹, Anusha Sridharan¹, Yan Xu¹, Susan E Wert¹, Jeanne James³, Nicholas Udell⁴, Philipp J Thurner⁴, Jeffrey A Whitsett⁵.

Abstract

The SRY-box containing transcription factor Sox17 is required for endoderm formation and vascular morphogenesis during embryonic development. In the lung, Sox17 is expressed in mesenchymal progenitors of the embryonic pulmonary vasculature and is restricted to vascular endothelial cells in the mature lung. Conditional deletion of Sox17 in splanchnic mesenchyme-derivatives using Dermo1-Cre resulted in substantial loss of Sox17 from developing pulmonary vascular endothelial cells and caused pulmonary vascular abnormalities before birth, including pulmonary vein varices, enlarged arteries, and decreased perfusion of the microvasculature. While survival of Dermo1-Cre;Sox17Δ/Δ mice (herein termed Sox17Δ/Δ) was unaffected at E18.5, most Sox17Δ/Δ mice died by 3 weeks of age. After birth, the density of the pulmonary microvasculature was decreased in association with alveolar simplification, biventricular cardiac hypertrophy, and valvular regurgitation. The severity of the postnatal cardiac phenotype was correlated with the severity of pulmonary vasculature abnormalities. Sox17 is required for normal formation of the pulmonary vasculature and postnatal cardiovascular homeostasis.

Entities: Chemical Disease Gene Species

Keywords: Dermo1-Cre; Endothelial; Lung; Sox17; Vascular morphogenesis

Mesh：

Substances：

Year: 2014 PMID： 24418654 PMCID： PMC4422074 DOI： 10.1016/j.ydbio.2013.11.018

Source DB: PubMed Journal: Dev Biol ISSN： 0012-1606 Impact factor: 3.582

38 in total

1. Sox17 dependence distinguishes the transcriptional regulation of fetal from adult hematopoietic stem cells.

Authors: Injune Kim; Thomas L Saunders; Sean J Morrison
Journal: Cell Date: 2007-07-26 Impact factor: 41.582

2. An improved method for three-dimensional reconstruction of protein expression patterns in intact mouse and chicken embryos and organs.

Authors: Jonas Ahnfelt-Rønne; Mette C Jørgensen; Jacob Hald; Ole D Madsen; Palle Serup; Jacob Hecksher-Sørensen
Journal: J Histochem Cytochem Date: 2007-05-03 Impact factor: 2.479

3. Generation of a mouse line expressing Sox17-driven Cre recombinase with specific activity in arteries.

Authors: W Perry Liao; Lena Uetzmann; Ingo Burtscher; Heiko Lickert
Journal: Genesis Date: 2009-07 Impact factor: 2.487

4. Mesodermal Pten inactivation leads to alveolar capillary dysplasia- like phenotype.

Authors: Caterina Tiozzo; Gianni Carraro; Denise Al Alam; Sheryl Baptista; Soula Danopoulos; Aimin Li; Maria Lavarreda-Pearce; Changgong Li; Stijn De Langhe; Belinda Chan; Zea Borok; Saverio Bellusci; Parviz Minoo
Journal: J Clin Invest Date: 2012-11 Impact factor: 14.808

5. Early expression of endomucin on endothelium of the mouse embryo and on putative hematopoietic clusters in the dorsal aorta.

Authors: G Brachtendorf; A Kuhn; U Samulowitz; R Knorr; E Gustafsson; A J Potocnik; R Fässler; D Vestweber
Journal: Dev Dyn Date: 2001-11 Impact factor: 3.780

6. Cardiac and skeletal muscle defects in a mouse model of human Barth syndrome.

Authors: Devrim Acehan; Frederic Vaz; Riekelt H Houtkooper; Jeanne James; Vicky Moore; Chonan Tokunaga; Willem Kulik; Janaka Wansapura; Matthew J Toth; Arnold Strauss; Zaza Khuchua
Journal: J Biol Chem Date: 2010-11-09 Impact factor: 5.157

7. Sox17 promotes tumor angiogenesis and destabilizes tumor vessels in mice.

Authors: Hanseul Yang; Sungsu Lee; Seungjoo Lee; Kangsan Kim; Yeseul Yang; Jeong Hoon Kim; Ralf H Adams; James M Wells; Sean J Morrison; Gou Young Koh; Injune Kim
Journal: J Clin Invest Date: 2012-12-17 Impact factor: 14.808

8. Sox18 and Sox7 play redundant roles in vascular development.

Authors: Solei Cermenati; Silvia Moleri; Simona Cimbro; Paola Corti; Luca Del Giacco; Roberta Amodeo; Elisabetta Dejana; Peter Koopman; Franco Cotelli; Monica Beltrame
Journal: Blood Date: 2007-12-19 Impact factor: 22.113

9. Zebrafish Sox7 and Sox18 function together to control arterial-venous identity.

Authors: Hélène Pendeville; Marie Winandy; Isabelle Manfroid; Olivier Nivelles; Patrick Motte; Vincent Pasque; Bernard Peers; Ingrid Struman; Joseph A Martial; Marianne L Voz
Journal: Dev Biol Date: 2008-02-07 Impact factor: 3.582

10. Canonical Notch signaling in the developing lung is required for determination of arterial smooth muscle cells and selection of Clara versus ciliated cell fate.

Authors: Mitsuru Morimoto; Zhenyi Liu; Hui-Teng Cheng; Niki Winters; David Bader; Raphael Kopan
Journal: J Cell Sci Date: 2010-01-15 Impact factor: 5.285

25 in total

Sox17 is required for normal pulmonary vascular morphogenesis.

1. Sox17 dependence distinguishes the transcriptional regulation of fetal from adult hematopoietic stem cells.

2. An improved method for three-dimensional reconstruction of protein expression patterns in intact mouse and chicken embryos and organs.

3. Generation of a mouse line expressing Sox17-driven Cre recombinase with specific activity in arteries.

4. Mesodermal Pten inactivation leads to alveolar capillary dysplasia- like phenotype.

5. Early expression of endomucin on endothelium of the mouse embryo and on putative hematopoietic clusters in the dorsal aorta.

6. Cardiac and skeletal muscle defects in a mouse model of human Barth syndrome.

7. Sox17 promotes tumor angiogenesis and destabilizes tumor vessels in mice.

8. Sox18 and Sox7 play redundant roles in vascular development.

9. Zebrafish Sox7 and Sox18 function together to control arterial-venous identity.

10. Canonical Notch signaling in the developing lung is required for determination of arterial smooth muscle cells and selection of Clara versus ciliated cell fate.

1. Conditional deletion of Sox17 reveals complex effects on uterine adenogenesis and function.

Review 2. Building and Regenerating the Lung Cell by Cell.

3. Decreased expression of SOX17 is associated with tumor progression and poor prognosis in breast cancer.

Review 4. Genetics and Other Omics in Pediatric Pulmonary Arterial Hypertension.

Review 5. SOXopathies: Growing Family of Developmental Disorders Due to SOX Mutations.

6. Endothelial TWIST1 promotes pathological ocular angiogenesis.

Review 7. 'There and Back Again'-Forward Genetics and Reverse Phenotyping in Pulmonary Arterial Hypertension.

8. Taiji-reprogram: a framework to uncover cell-type specific regulators and predict cellular reprogramming cocktails.

Review 9. Molecular genetic framework underlying pulmonary arterial hypertension.

Review 10. Genes that drive the pathobiology of pediatric pulmonary arterial hypertension.