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Literature DB >> 34714692

Age and sex dependency of thoracic aortopathy in a mouse model of Marfan syndrome.

Nazli Gharraee¹, Yujian Sun², Joseph A Swisher³, Susan M Lessner^1,4.

Abstract

Thoracic aortic aneurysm is one of the manifestations of Marfan syndrome (MFS) that is known to affect men more severely than women. However, the incidence of MFS is similar between men and women. The aim of this study is to show that during pathological aortic dilation, sex-dependent severity of thoracic aortopathy in a mouse model of MFS translates into sex-dependent alterations in cells and matrix of the ascending aorta, consequently affecting aortic biomechanics. Fibrillin-1 C1041G/+ (Het) mice were used as a mouse model of MFS. Ultrasound measurements from 3 to 12 mo showed increased aortic diameter in Het aorta, with larger percentage increase in diameter for males compared with females. Immunohistochemistry showed decreased contractile smooth muscle cells in Het aortic wall compared with healthy aorta, which was accompanied by decreased contractility measured by wire myography. Elastin autofluorescence, second-harmonic generation microscopy of collagen fibers, and passive biomechanical assessments using myography showed more severe damage to elastin fibers, increased medial fibrosis, and increased stiffness of the aortic wall in MFS males but not females. Male and female Het mice showed increased expression of Sca-1-positive adventitial progenitor cells versus controls at young ages. In agreement with clinical data, Het mice demonstrate sex-dependent severity of thoracic aortopathy. It was also shown that aging exacerbates the disease state especially for males. Our findings suggest that female mice are protected from progression of aortic dilation at early ages, leading to a lag in aneurysm growth.NEW & NOTEWORTHY Male Fbn1C1041G/+ mice show more severe thoracic aortic changes compared with females, especially at 12 mo of age. Up to 6 mo of age, Sca-1+ smooth muscle progenitor cells are more abundant in the adventitia of both male and female Fbn1 Het mice compared with wild types (WTs). Male and female Het mice show similar patterns of expression of Sca-1+ cells at early ages.

Entities: Chemical

Keywords: Marfan syndrome; progenitor cells; sex dependency; thoracic aortic aneurysm; vascular remodeling

Mesh：

Substances：

Year: 2021 PMID： 34714692 PMCID： PMC8698500 DOI： 10.1152/ajpheart.00255.2021

Source DB: PubMed Journal: Am J Physiol Heart Circ Physiol ISSN： 0363-6135 Impact factor: 4.733

51 in total

1. Origin of Matrix-Producing Cells That Contribute to Aortic Fibrosis in Hypertension.

Authors: Jing Wu; Kim Ramil C Montaniel; Mohamed A Saleh; Liang Xiao; Wei Chen; Gary K Owens; Jay D Humphrey; Mark W Majesky; David T Paik; Antonis K Hatzopoulos; Meena S Madhur; David G Harrison
Journal: Hypertension Date: 2015-12-22 Impact factor: 10.190

Review 2. Genetic basis of thoracic aortic aneurysms and dissections: focus on smooth muscle cell contractile dysfunction.

Authors: Dianna M Milewicz; Dong-Chuan Guo; Van Tran-Fadulu; Andrea L Lafont; Christina L Papke; Sakiko Inamoto; Carrie S Kwartler; Hariyadarshi Pannu
Journal: Annu Rev Genomics Hum Genet Date: 2008 Impact factor: 8.929

3. Sca-1⁺ cardiac fibroblasts promote development of heart failure.

Authors: Guobao Chen; William Bracamonte-Baran; Nicola L Diny; Xuezhou Hou; Monica V Talor; Kai Fu; Yue Liu; Giovanni Davogustto; Hernan Vasquez; Heinrich Taegtmeyer; O Howard Frazier; Ari Waisman; Simon J Conway; Fengyi Wan; Daniela Čiháková
Journal: Eur J Immunol Date: 2018-07-18 Impact factor: 5.532

4. Impact of Pathogenic FBN1 Variant Types on the Progression of Aortic Disease in Patients With Marfan Syndrome.

Authors: Norifumi Takeda; Ryo Inuzuka; Sonoko Maemura; Hiroyuki Morita; Kan Nawata; Daishi Fujita; Yuki Taniguchi; Haruo Yamauchi; Hiroki Yagi; Masayoshi Kato; Hiroshi Nishimura; Yoichiro Hirata; Yuichi Ikeda; Hidetoshi Kumagai; Eisuke Amiya; Hironori Hara; Takayuki Fujiwara; Hiroshi Akazawa; Jun-Ichi Suzuki; Yasushi Imai; Ryozo Nagai; Shinichi Takamoto; Yasunobu Hirata; Minoru Ono; Issei Komuro
Journal: Circ Genom Precis Med Date: 2018-06

5. Cell biology. Dysfunctional mechanosensing in aneurysms.

Authors: Jay D Humphrey; Dianna M Milewicz; George Tellides; Martin A Schwartz
Journal: Science Date: 2014-05-02 Impact factor: 47.728

6. Vascular smooth muscle cell phenotypic changes in patients with Marfan syndrome.

Authors: Eva Crosas-Molist; Thayna Meirelles; Judit López-Luque; Carla Serra-Peinado; Javier Selva; Laia Caja; Darya Gorbenko Del Blanco; Juan José Uriarte; Esther Bertran; Yolanda Mendizábal; Vanessa Hernández; Carolina García-Calero; Oscar Busnadiego; Enric Condom; David Toral; Manel Castellà; Alberto Forteza; Daniel Navajas; Elisabet Sarri; Fernando Rodríguez-Pascual; Harry C Dietz; Isabel Fabregat; Gustavo Egea
Journal: Arterioscler Thromb Vasc Biol Date: 2015-01-15 Impact factor: 8.311

7. Associations of Age and Sex With Marfan Phenotype: The National Heart, Lung, and Blood Institute GenTAC (Genetically Triggered Thoracic Aortic Aneurysms and Cardiovascular Conditions) Registry.

Authors: Mary J Roman; Richard B Devereux; Liliana R Preiss; Federico M Asch; Kim A Eagle; Kathryn W Holmes; Scott A LeMaire; Cheryl L Maslen; Dianna M Milewicz; Shaine A Morris; Siddharth K Prakash; Reed E Pyeritz; William J Ravekes; Ralph V Shohet; Howard K Song; Jonathan W Weinsaft
Journal: Circ Cardiovasc Genet Date: 2017-06

Age and sex dependency of thoracic aortopathy in a mouse model of Marfan syndrome.

1. Origin of Matrix-Producing Cells That Contribute to Aortic Fibrosis in Hypertension.

Review 2. Genetic basis of thoracic aortic aneurysms and dissections: focus on smooth muscle cell contractile dysfunction.

3. Sca-1⁺ cardiac fibroblasts promote development of heart failure.

4. Impact of Pathogenic FBN1 Variant Types on the Progression of Aortic Disease in Patients With Marfan Syndrome.

5. Cell biology. Dysfunctional mechanosensing in aneurysms.

6. Vascular smooth muscle cell phenotypic changes in patients with Marfan syndrome.

7. Associations of Age and Sex With Marfan Phenotype: The National Heart, Lung, and Blood Institute GenTAC (Genetically Triggered Thoracic Aortic Aneurysms and Cardiovascular Conditions) Registry.

8. Evidence for a critical contribution of haploinsufficiency in the complex pathogenesis of Marfan syndrome.

Review 9. Stem cell aging: mechanisms, regulators and therapeutic opportunities.

10. Abundant progenitor cells in the adventitia contribute to atherosclerosis of vein grafts in ApoE-deficient mice.

1. Progressive Microstructural Deterioration Dictates Evolving Biomechanical Dysfunction in the Marfan Aorta.