Your search keyword '"Kwartler CS"' showing total 30 results

1. Use of iPSC-Derived Smooth Muscle Cells to Model Physiology and Pathology.

Author

Kwartler CS and Esparza Pinelo JE

Subjects

Humans, Animals, Phenotype, Muscle, Smooth, Vascular pathology, Muscle, Smooth, Vascular metabolism, Cell Lineage, Induced Pluripotent Stem Cells metabolism, Induced Pluripotent Stem Cells pathology, Myocytes, Smooth Muscle pathology, Myocytes, Smooth Muscle metabolism, Cell Differentiation

Abstract

The implementation of human induced pluripotent stem cell (hiPSC) models has introduced an additional tool for identifying molecular mechanisms of disease that complement animal models. Patient-derived or CRISPR/Cas9-edited induced pluripotent stem cells differentiated into smooth muscle cells (SMCs) have been leveraged to discover novel mechanisms, screen potential therapeutic strategies, and model in vivo development. The field has evolved over almost 15 years of research using hiPSC-SMCs and has made significant strides toward overcoming initial challenges such as the lineage specificity of SMC phenotypes. However, challenges both specific (eg, the lack of specific markers to thoroughly validate hiPSC-SMCs) and general (eg, a lack of transparency and consensus around methodology in the field) remain. In this review, we highlight the recent successes and remaining challenges of the hiPSC-SMC model., Competing Interests: Disclosures None.

Published

2024

2. Pericentrin deficiency in smooth muscle cells augments atherosclerosis through HSF1-driven cholesterol biosynthesis and PERK activation.

Author

Majumder S, Chattopadhyay A, Wright JM, Guan P, Buja LM, Kwartler CS, and Milewicz DM

Subjects

Animals, Humans, Mice, Cholesterol metabolism, Myocytes, Smooth Muscle metabolism, Atherosclerosis pathology, Hydroxymethylglutaryl-CoA Reductase Inhibitors, Plaque, Atherosclerotic pathology

Abstract

Microcephalic osteodysplastic primordial dwarfism type II (MOPDII) is caused by biallelic loss-of-function variants in pericentrin (PCNT), and premature coronary artery disease (CAD) is a complication of the syndrome. Histopathology of coronary arteries from patients with MOPDII who died of CAD in their 20s showed extensive atherosclerosis. Hyperlipidemic mice with smooth muscle cell-specific (SMC-specific) Pcnt deficiency (PcntSMC-/-) exhibited significantly greater atherosclerotic plaque burden compared with similarly treated littermate controls despite similar serum lipid levels. Loss of PCNT in SMCs induced activation of heat shock factor 1 (HSF1) and consequently upregulated the expression and activity of HMG-CoA reductase (HMGCR), the rate-limiting enzyme in cholesterol biosynthesis. The increased cholesterol biosynthesis in PcntSMC-/- SMCs augmented PERK signaling and phenotypic modulation compared with control SMCs. Treatment with the HMGCR inhibitor, pravastatin, blocked the augmented SMC modulation and reduced plaque burden in hyperlipidemic PcntSMC-/- mice to that of control mice. These data support the notion that Pcnt deficiency activates cellular stress to increase SMC modulation and plaque burden, and targeting this pathway with statins in patients with MOPDII has the potential to reduce CAD in these individuals. The molecular mechanism uncovered further emphasizes SMC cytosolic stress and HSF1 activation as a pathway driving atherosclerotic plaque formation independently of cholesterol levels.

Published

2023

3. Augmenting Mitochondrial Respiration in Immature Smooth Muscle Cells with an ACTA2 Pathogenic Variant Mitigates Moyamoya-like Cerebrovascular Disease.

Author

Kaw A, Wu T, Starosolski Z, Zhou Z, Pedroza AJ, Majumder S, Duan X, Kaw K, Pinelo JEE, Fischbein MP, Lorenzi PL, Tan L, Martinez SA, Mahmud I, Devkota L, Taegtmeyer H, Ghaghada KB, Marrelli SP, Kwartler CS, and Milewicz DM

Abstract

ACTA2 pathogenic variants altering arginine 179 cause childhood-onset strokes due to moyamoya disease (MMD)-like occlusion of the distal internal carotid arteries. A smooth muscle cell (SMC)-specific knock-in mouse model ( Acta2 SMC-R179C/+ ) inserted the mutation into 67% of aortic SMCs, whereas explanted SMCs were uniformly heterozygous. Acta2 R179C/+ SMCs fail to fully differentiate and maintain stem cell-like features, including high glycolytic flux, and increasing oxidative respiration (OXPHOS) with nicotinamide riboside (NR) drives the mutant SMCs to differentiate and decreases migration. Acta2 SMC-R179C/+ mice have intraluminal MMD-like occlusive lesions and strokes after carotid artery injury, whereas the similarly treated WT mice have no strokes and patent lumens. Treatment with NR prior to the carotid artery injury attenuates the strokes, MMD-like lumen occlusions, and aberrant vascular remodeling in the Acta2 SMC-R179C/+ mice. These data highlight the role of immature SMCs in MMD-associated occlusive disease and demonstrate that altering SMC metabolism to drive quiescence of Acta2 R179C/+ SMCs attenuates strokes and aberrant vascular remodeling in the Acta2 SMC-R179C/+ mice.

Published

2023

4. Nuclear Smooth Muscle α-actin Participates in Vascular Smooth Muscle Cell Differentiation.

Author

Kwartler CS, Pedroza AJ, Kaw A, Guan P, Ma S, Duan XY, Kernell C, Wang C, Pinelo JEE, Bowen MSB, Chen J, Zhong Y, Sinha S, Shen X, Fischbein MP, and Milewicz DM

Abstract

Missense variants throughout ACTA2 , encoding smooth muscle α-actin (αSMA), predispose to adult-onset thoracic aortic disease, but variants disrupting arginine 179 (R179) lead to Smooth Muscle Dysfunction Syndrome (SMDS) characterized by diverse childhood-onset vascular diseases. Here we show that αSMA localizes to the nucleus in wildtype (WT) smooth muscle cells (SMCs), enriches in the nucleus with SMC differentiation, and associates with chromatin remodeling complexes and SMC contractile gene promotors. The ACTA2 p.R179 αSMA variant shows decreased nuclear localization. Primary SMCs from Acta2 SMC-R179C/+ mice are less differentiated than WT SMCs in vitro and in vivo and have global changes in chromatin accessibility. Induced pluripotent stem cells from patients with ACTA2 p.R179 variants fail to fully differentiate from neuroectodermal progenitor cells to SMCs, and single-cell transcriptomic analyses of an ACTA2 p.R179H patient's aortic tissue show increased SMC plasticity. Thus, nuclear αSMA participates in SMC differentiation, and loss of this nuclear activity occurs with ACTA2 p.R179 pathogenic variants., Competing Interests: Declaration of Interests The authors declare no competing interests.

Published

2023

5. Smooth muscle α-actin missense variant promotes atherosclerosis through modulation of intracellular cholesterol in smooth muscle cells.

Author

Kaw K, Chattopadhyay A, Guan P, Chen J, Majumder S, Duan XY, Ma S, Zhang C, Kwartler CS, and Milewicz DM

Subjects

Mice, Animals, Actins metabolism, Mice, Knockout, ApoE, Cholesterol metabolism, Myocytes, Smooth Muscle metabolism, Myocytes, Smooth Muscle pathology, Muscle, Smooth metabolism, Muscle, Smooth pathology, Apolipoproteins E genetics, Apolipoproteins E metabolism, Mice, Inbred C57BL, Mice, Knockout, Plaque, Atherosclerotic complications, Atherosclerosis etiology, Hyperlipidemias complications

Abstract

Aims: The variant p.Arg149Cys in ACTA2, which encodes smooth muscle cell (SMC)-specific α-actin, predisposes to thoracic aortic disease and early onset coronary artery disease in individuals without cardiovascular risk factors. This study investigated how this variant drives increased atherosclerosis., Methods and Results: Apoe-/- mice with and without the variant were fed a high-fat diet for 12 weeks, followed by evaluation of atherosclerotic plaque formation and single-cell transcriptomics analysis. SMCs explanted from Acta2R149C/+ and wildtype (WT) ascending aortas were used to investigate atherosclerosis-associated SMC phenotypic modulation. Hyperlipidemic Acta2R149C/+Apoe-/- mice have a 2.5-fold increase in atherosclerotic plaque burden compared to Apoe-/- mice with no differences in serum lipid levels. At the cellular level, misfolding of the R149C α-actin activates heat shock factor 1, which increases endogenous cholesterol biosynthesis and intracellular cholesterol levels through increased HMG-CoA reductase (HMG-CoAR) expression and activity. The increased cellular cholesterol in Acta2R149C/+ SMCs induces endoplasmic reticulum stress and activates PERK-ATF4-KLF4 signaling to drive atherosclerosis-associated phenotypic modulation in the absence of exogenous cholesterol, while WT cells require higher levels of exogenous cholesterol to drive phenotypic modulation. Treatment with the HMG-CoAR inhibitor pravastatin successfully reverses the increased atherosclerotic plaque burden in Acta2R149C/+Apoe-/- mice., Conclusion: These data establish a novel mechanism by which a pathogenic missense variant in a smooth muscle-specific contractile protein predisposes to atherosclerosis in individuals without hypercholesterolemia or other risk factors. The results emphasize the role of increased intracellular cholesterol levels in driving SMC phenotypic modulation and atherosclerotic plaque burden., (© The Author(s) 2023. Published by Oxford University Press on behalf of the European Society of Cardiology.)

Published

2023

6. Nuclear Smooth Muscle α-actin in Vascular Smooth Muscle Cell Differentiation.

Author

Kwartler CS, Pedroza AJ, Kaw A, Guan P, Ma S, Duan XY, Kernell C, Wang C, Pinelo JEE, Borthwick MS, Chen J, Zhong Y, Sinha S, Shen X, Fischbein MP, and Milewicz DM

Abstract

Missense variants throughout ACTA2 , encoding smooth muscle α-actin (αSMA), predispose to adult onset thoracic aortic disease, but variants disrupting arginine 179 (R179) lead to Smooth Muscle Dysfunction Syndrome (SMDS) characterized by childhood-onset diverse vascular diseases. Our data indicate that αSMA localizes to the nucleus in wildtype (WT) smooth muscle cells (SMCs), enriches in the nucleus with SMC differentiation, and associates with chromatin remodeling complexes and SMC contractile gene promotors, and the ACTA2 p.R179 variant decreases nuclear localization of αSMA. SMCs explanted from a SMC-specific conditional knockin mouse model, Acta2 SMC-R179/+ , are less differentiated than WT SMCs, both in vitro and in vivo , and have global changes in chromatin accessibility. Induced pluripotent stem cells from patients with ACTA2 p.R179 variants fail to fully differentiate from neural crest cells to SMCs, and single cell transcriptomic analyses of an ACTA2 p.R179H patient's aortic tissue shows increased SMC plasticity. Thus, nuclear αSMA participates in SMC differentiation and loss of this nuclear activity occurs with ACTA2 p.R179 pathogenic variants., Competing Interests: Declaration of Interests The authors declare no competing interests.

Published

2023

7. Mosaicism for the smooth muscle cell (SMC)-specific knock-in of the Acta2 R179C pathogenic variant: Implications for gene editing therapies.

Author

Kaw A, Pedroza AJ, Chattopadhyay A, Pinard A, Guo D, Kaw K, Zhou Z, Shad R, Fischbein MP, Kwartler CS, and Milewicz DM

Subjects

Actins genetics, Gene Editing, Humans, Myocytes, Smooth Muscle pathology, Aortic Aneurysm, Thoracic pathology, Mosaicism

Published

2022

8. Expanding ACTA2 genotypes with corresponding phenotypes overlapping with smooth muscle dysfunction syndrome.

Author

Kaw A, Kaw K, Hostetler EM, Beleza-Meireles A, Smith-Collins A, Armstrong C, Scurr I, Cotts T, Aatre R, Bamshad MJ, Earl D, Groner A, Agre K, Raveh Y, Kwartler CS, and Milewicz DM

Subjects

Heterozygote, Humans, Muscle, Smooth, Mutation, Phenotype, Actins genetics, Aortic Aneurysm, Thoracic diagnosis, Aortic Aneurysm, Thoracic genetics, Cerebrovascular Disorders, Ductus Arteriosus, Patent genetics, Moyamoya Disease genetics

Abstract

Pathogenic variants in ACTA2, encoding smooth muscle α-actin, predispose to thoracic aortic aneurysms and dissections. ACTA2 variants altering arginine 179 predispose to a more severe, multisystemic disease termed smooth muscle dysfunction syndrome (SMDS; OMIM 613834). Vascular complications of SMDS include patent ductus arteriosus (PDA) or aortopulmonary window, early-onset thoracic aortic disease (TAD), moyamoya-like cerebrovascular disease, and primary pulmonary hypertension. Patients also have dysfunction of other smooth muscle-dependent systems, including congenital mydriasis, hypotonic bladder, and gut hypoperistalsis. Here, we describe five patients with novel heterozygous ACTA2 missense variants, p.Arg179Gly, p.Met46Arg, p.Thr204Ile, p.Arg39Cys, and p.Ile66Asn, who have clinical complications that align or overlap with SMDS. Patients with the ACTA2 p.Arg179Gly and p.Thr204Ile variants display classic features of SMDS. The patient with the ACTA2 p.Met46Arg variant exhibits exclusively vascular complications of SMDS, including early-onset TAD, PDA, and moyamoya-like cerebrovascular disease. The patient with the ACTA2 p.Ile66Asn variant has an unusual vascular complication, a large fusiform internal carotid artery aneurysm. The patient with the ACTA2 p.Arg39Cys variant has pulmonary, gastrointestinal, and genitourinary complications of SMDS but no vascular manifestations. Identifying pathogenic ACTA2 variants associated with features of SMDS is critical for aggressive surveillance and management of vascular and nonvascular complications and delineating the molecular pathogenesis of SMDS., (© 2022 Wiley Periodicals LLC.)

Published

2022

9. Preventing Cholesterol-Induced Perk (Protein Kinase RNA-Like Endoplasmic Reticulum Kinase) Signaling in Smooth Muscle Cells Blocks Atherosclerotic Plaque Formation.

Author

Chattopadhyay A, Guan P, Majumder S, Kaw K, Zhou Z, Zhang C, Prakash SK, Kaw A, Buja LM, Kwartler CS, and Milewicz DM

Subjects

Animals, Cells, Cultured, Cholesterol metabolism, Endoplasmic Reticulum metabolism, Male, Mice, Muscle, Smooth, Vascular cytology, Atherosclerosis genetics, Atherosclerosis metabolism, Atherosclerosis prevention & control, Myocytes, Smooth Muscle metabolism, Plaque, Atherosclerotic metabolism, eIF-2 Kinase metabolism

Abstract

Background: Vascular smooth muscle cells (SMCs) undergo complex phenotypic modulation with atherosclerotic plaque formation in hyperlipidemic mice, which is characterized by de-differentiation and heterogeneous increases in the expression of macrophage, fibroblast, osteogenic, and stem cell markers. An increase of cellular cholesterol in SMCs triggers similar phenotypic changes in vitro with exposure to free cholesterol due to cholesterol entering the endoplasmic reticulum, triggering endoplasmic reticulum stress and activating Perk (protein kinase RNA-like endoplasmic reticulum kinase) signaling., Methods: We generated an SMC-specific Perk knockout mouse model, induced hyperlipidemia in the mice by AAV- PCSK9 DY injection, and subjected them to a high-fat diet. We then assessed atherosclerotic plaque formation and performed single-cell transcriptomic studies using aortic tissue from these mice., Results: SMC-specific deletion of Perk reduces atherosclerotic plaque formation in male hyperlipidemic mice by 80%. Single-cell transcriptomic data identify 2 clusters of modulated SMCs in hyperlipidemic mice, one of which is absent when Perk is deleted in SMCs. The 2 modulated SMC clusters have significant overlap of transcriptional changes, but the Perk-dependent cluster uniquely shows a global decrease in the number of transcripts. SMC-specific Perk deletion also prevents migration of both contractile and modulated SMCs from the medial layer of the aorta., Conclusions: Our results indicate that hypercholesterolemia drives both Perk-dependent and Perk-independent SMC modulation and that deficiency of Perk significantly blocks atherosclerotic plaque formation.

Published

2022

10. Aortic root dilatation and dilated cardiomyopathy in an adult with Tatton-Brown-Rahman syndrome.

Author

Cecchi AC, Haidar A, Marin I, Kwartler CS, Prakash SK, and Milewicz DM

Subjects

Adult, DNA (Cytosine-5-)-Methyltransferases genetics, DNA Methyltransferase 3A, Dilatation, Humans, Mutation, Aortic Diseases complications, Aortic Diseases diagnosis, Aortic Diseases genetics, Cardiomyopathy, Dilated complications, Cardiomyopathy, Dilated diagnosis, Cardiomyopathy, Dilated genetics, Intellectual Disability genetics, Marfan Syndrome complications, Marfan Syndrome diagnosis, Marfan Syndrome genetics

Abstract

Tatton-Brown-Rahman syndrome is an autosomal dominant overgrowth syndrome caused by pathogenic DNMT3A variants in the germline. Clinical findings of tall stature due to postnatal overgrowth, intellectual disability, and characteristic facial features, are the most consistent findings observed in patients with Tatton-Brown-Rahman syndrome (TBRS). Since the syndrome was first described in 2014, an expanding spectrum of neuropsychiatric, musculoskeletal, neurological, and cardiovascular manifestations have been reported. However, most TBRS cases described in the literature are children with de novo DNMT3A variants, signaling a need to better characterize the phenotypes in adults. In this report, we describe a 34 year old referred to genetics for possible Marfan syndrome with aortic root dilatation, mitral valve prolapse, and dilated cardiomyopathy, who was diagnosed with TBRS due to a heterozygous de novo DNMT3A variant. This represents the third reported TBRS case with aortic root dilation and the second with cardiomyopathy. Collectively, these data provide evidence for an association with aortic disease and cardiomyopathy, highlight the clinical overlap with Marfan syndrome, and suggest that cardiovascular surveillance into adulthood is indicated., (© 2021 Wiley Periodicals LLC.)

Published

2022

11. Resistance of Acta2 R149C/+ mice to aortic disease is associated with defective release of mutant smooth muscle α-actin from the chaperonin-containing TCP1 folding complex.

Author

Chen J, Kaw K, Lu H, Fagnant PM, Chattopadhyay A, Duan XY, Zhou Z, Ma S, Liu Z, Huang J, Kamm K, Stull JT, Kwartler CS, Trybus KM, and Milewicz DM

Subjects

Actins metabolism, Animals, Aorta metabolism, Aorta pathology, Aortic Diseases metabolism, Aortic Diseases pathology, Mice, Mice, Inbred C57BL, Mutation, Missense, Actins genetics, Aortic Diseases genetics, Chaperonin Containing TCP-1 metabolism, Point Mutation

Abstract

Pathogenic variants of the gene for smooth muscle α-actin (ACTA2), which encodes smooth muscle (SM) α-actin, predispose to heritable thoracic aortic disease. The ACTA2 variant p.Arg149Cys (R149C) is the most common alteration; however, only 60% of carriers have a dissection or undergo repair of an aneurysm by 70 years of age. A mouse model of ACTA2 p.Arg149Cys was generated using CRISPR/Cas9 technology to determine the etiology of reduced penetrance. Acta2 R149C/+ mice had significantly decreased aortic contraction compared with WT mice but did not form aortic aneurysms or dissections when followed to 24 months, even when hypertension was induced. In vitro motility assays found decreased interaction of mutant SM α-actin filaments with SM myosin. Polymerization studies using total internal reflection fluorescence microscopy showed enhanced nucleation of mutant SM α-actin by formin, which correlated with disorganized and reduced SM α-actin filaments in Acta2 R149C/+ smooth muscle cells (SMCs). However, the most prominent molecular defect was the increased retention of mutant SM α-actin in the chaperonin-containing t-complex polypeptide folding complex, which was associated with reduced levels of mutant compared with WT SM α-actin in Acta2 R149C/+ SMCs. These data indicate that Acta2 R149C/+ mice do not develop thoracic aortic disease despite decreased contraction of aortic segments and disrupted SM α-actin filament formation and function in Acta2 R149C/+ SMCs. Enhanced binding of mutant SM α-actin to chaperonin-containing t-complex polypeptide decreases the mutant actin versus WT monomer levels in Acta2 R149C/+ SMCs, thus minimizing the effect of the mutation on SMC function and potentially preventing aortic disease in the Acta2 R149C/+ mice., Competing Interests: Conflict of interest The authors declare that they have no conflicts of interest with the contents of this article., (Copyright © 2021 The Authors. Published by Elsevier Inc. All rights reserved.)

Published

2021

12. Cholesterol-Induced Phenotypic Modulation of Smooth Muscle Cells to Macrophage/Fibroblast-like Cells Is Driven by an Unfolded Protein Response.

Author

Chattopadhyay A, Kwartler CS, Kaw K, Li Y, Kaw A, Chen J, LeMaire SA, Shen YH, and Milewicz DM

Subjects

Activating Transcription Factor 4 metabolism, Animals, Atherosclerosis metabolism, Atherosclerosis pathology, Cell Line, Endoplasmic Reticulum Stress drug effects, Eukaryotic Initiation Factor-2 metabolism, Female, Fibroblasts metabolism, Fibroblasts pathology, Kruppel-Like Factor 4, Kruppel-Like Transcription Factors metabolism, Macrophages metabolism, Macrophages pathology, Male, Mice, Inbred C57BL, Muscle, Smooth, Vascular metabolism, Muscle, Smooth, Vascular pathology, Myocytes, Smooth Muscle metabolism, Myocytes, Smooth Muscle pathology, Phenotype, Plaque, Atherosclerotic, eIF-2 Kinase metabolism, Mice, Cell Transdifferentiation drug effects, Cholesterol toxicity, Fibroblasts drug effects, Macrophages drug effects, Muscle, Smooth, Vascular drug effects, Myocytes, Smooth Muscle drug effects, Unfolded Protein Response drug effects

Abstract

Objective: Vascular smooth muscle cells (SMCs) dedifferentiate and initiate expression of macrophage markers with cholesterol exposure. This phenotypic switching is dependent on the transcription factor Klf4 (Krüppel-like factor 4). We investigated the molecular pathway by which cholesterol induces SMC phenotypic switching. Approach and Results: With exposure to free cholesterol, SMCs decrease expression of contractile markers, activate Klf4, and upregulate a subset of macrophage and fibroblast markers characteristic of modulated SMCs that appear with atherosclerotic plaque formation. These phenotypic changes are associated with activation of all 3 pathways of the endoplasmic reticulum unfolded protein response (UPR), Perk (protein kinase RNA-like endoplasmic reticulum kinase), Ire (inositol-requiring enzyme) 1α, and Atf (activating transcription factor) 6. Blocking the movement of cholesterol from the plasma membrane to the endoplasmic reticulum prevents free cholesterol-induced UPR, Klf4 activation, and upregulation of the majority of macrophage and fibroblast markers. Cholesterol-induced phenotypic switching is also prevented by global UPR inhibition or specific inhibition of Perk signaling. Exposure to chemical UPR inducers, tunicamycin and thapsigargin, is sufficient to induce these same phenotypic transitions. Finally, analysis of published single-cell RNA sequencing data during atherosclerotic plaque formation in hyperlipidemic mice provides preliminary in vivo evidence of a role of UPR activation in modulated SMCs., Conclusions: Our data demonstrate that UPR is necessary and sufficient to drive phenotypic switching of SMCs to cells that resemble modulated SMCs found in atherosclerotic plaques. Preventing a UPR in hyperlipidemic mice diminishes atherosclerotic burden, and our data suggest that preventing SMC transition to dedifferentiated cells expressing macrophage and fibroblast markers contributes to this decreased plaque burden.

Published

2021

13. Stromal β-catenin activation impacts nephron progenitor differentiation in the developing kidney and may contribute to Wilms tumor.

Author

Drake KA, Chaney CP, Das A, Roy P, Kwartler CS, Rakheja D, and Carroll TJ

Subjects

Animals, Base Sequence, Body Patterning genetics, Cell Lineage genetics, Epithelium embryology, Forkhead Transcription Factors metabolism, Gene Expression Regulation, Neoplastic, Humans, Integrases metabolism, Mesoderm embryology, Mice, Mutation genetics, Nephrons metabolism, Organogenesis genetics, Osteogenesis genetics, Stromal Cells metabolism, Stromal Cells pathology, Transcriptome genetics, Wilms Tumor genetics, beta Catenin genetics, Cell Differentiation genetics, Nephrons pathology, Stem Cells metabolism, Wilms Tumor metabolism, Wilms Tumor pathology, beta Catenin metabolism

Abstract

Wilms' tumor (WT) morphologically resembles the embryonic kidney, consisting of blastema, epithelial and stromal components, suggesting tumors arise from the dysregulation of normal development. β-Catenin activation is observed in a significant proportion of WTs; however, much remains to be understood about how it contributes to tumorigenesis. Although activating β-catenin mutations are observed in both blastema and stromal components of WT, current models assume that activation in the blastemal lineage is causal. Paradoxically, studies performed in mice suggest that activation of β-catenin in the nephrogenic lineage results in loss of nephron progenitor cell (NPC) renewal, a phenotype opposite to WT. Here, we show that activation of β-catenin in the stromal lineage non-autonomously prevents the differentiation of NPCs. Comparisons of the transcriptomes of kidneys expressing an activated allele of β-catenin in the stromal or nephron progenitor cells reveals that human WT more closely resembles the stromal-lineage mutants. These findings suggest that stromal β-catenin activation results in histological and molecular features of human WT, providing insights into how alterations in the stromal microenvironment may play an active role in tumorigenesis., Competing Interests: Competing interestsThe authors declare no competing or financial interests., (© 2020. Published by The Company of Biologists Ltd.)

Published

2020

14. Grange syndrome due to homozygous YY1AP1 missense rare variants.

Author

Ciuffetelli Alamo IV, Kwartler CS, Regalado ER, Afifi RO, Parkash S, Rideout A, Guo DC, and Milewicz DM

Subjects

Cell Line, Computed Tomography Angiography, Consanguinity, Female, Humans, Male, Tomography, X-Ray Computed, Arterial Occlusive Diseases diagnosis, Arterial Occlusive Diseases genetics, Bone and Bones abnormalities, Brachydactyly diagnosis, Brachydactyly genetics, Cell Cycle Proteins genetics, Genetic Association Studies methods, Genetic Predisposition to Disease, Heart Defects, Congenital diagnosis, Heart Defects, Congenital genetics, Homozygote, Hypertension diagnosis, Hypertension genetics, Mutation, Missense, Syndactyly diagnosis, Syndactyly genetics, Transcription Factors genetics

Abstract

Grange syndrome (OMIM 602531) is an autosomal recessive condition characterized by severe early onset vascular occlusive disease and variable penetrance of brachydactyly, syndactyly, bone fragility, and learning disabilities. Grange syndrome is caused by homozygous or compound heterozygous loss-of-function variants in the YYA1P1 gene. We report on the case of a 53-year old female with novel homozygous missense variants in YYA1P1 (c.1079C>T, p.Pro360Leu), presenting with a history of brachysyndactyly, hypertension, and ischemic stroke. Imaging studies revealed stenosis of the bilateral internal carotid with extensive collateralization of cerebral vessels in a moyamoya-like pattern, along with stenosis in the splenic, common hepatic, celiac, left renal, and superior mesenteric arteries. Functional studies conducted with the patient's dermal fibroblasts suggest that the p.Pro360Leu variant decreases the stability of the YY1AP1 protein. This is the first report of a missense variant associated with Grange syndrome characterized by later onset of vascular disease and a lack of developmental delay and bone fragility., (© 2019 Wiley Periodicals, Inc.)

Published

2019

15. Reversal of Aortic Enlargement Induced by Increased Biomechanical Forces Requires AT1R Inhibition in Conjunction With AT2R Activation.

Author

Zhou Z, Peters AM, Wang S, Janda A, Chen J, Zhou P, Arthur E, Kwartler CS, and Milewicz DM

Subjects

Angiotensin II Type 1 Receptor Blockers pharmacology, Angiotensin II Type 2 Receptor Blockers pharmacology, Animals, Aorta physiopathology, Aortic Aneurysm etiology, Aortic Aneurysm prevention & control, Aortitis drug therapy, Aortitis etiology, Aortitis physiopathology, Biomechanical Phenomena, Captopril pharmacology, Constriction, Hypertension complications, Hypertension physiopathology, Imidazoles pharmacology, Losartan pharmacology, Male, Mice, Mice, Inbred C57BL, Proto-Oncogene Mas, Proto-Oncogene Proteins agonists, Proto-Oncogene Proteins physiology, Pyridines pharmacology, Random Allocation, Receptors, G-Protein-Coupled agonists, Receptors, G-Protein-Coupled physiology, Renin-Angiotensin System drug effects, Renin-Angiotensin System physiology, Vascular Remodeling drug effects, Aortic Aneurysm physiopathology, Receptor, Angiotensin, Type 1 physiology, Receptor, Angiotensin, Type 2 physiology

Abstract

Objective- Pharmacological inhibition of the AT1R (angiotensin II type 1 receptor) with losartan can attenuate ascending aortic remodeling induced by transverse aortic constriction (TAC). In this study, we investigated the role of the AT2R (angiotensin II type 2 receptor) and MasR (Mas receptor) in TAC-induced ascending aortic dilation and remodeling. Approach and Results- Wild-type C57BL/6J mice were subjected to sham or TAC surgeries in the presence and absence of various drugs. Aortic diameters were assessed by echocardiography, central blood pressure was measured in the ascending aorta 2 weeks post-operation, and histology and gene expression analyses completed. An angiotensin-converting enzyme inhibitor, captopril, decreased systolic blood pressure to the same level as losartan but did not attenuate aortic dilation, adventitial inflammation, medial collagen deposition, elastin breakage, or Mmp9 (matrix metalloproteinase-9) expression when compared with TAC mice. In contrast, co-administration of captopril with an AT2R agonist, compound 21, attenuated aortic dilation, medial collagen content, elastin breaks, and Mmp9 expression, whereas co-administration of captopril with a MasR agonist (AVE0991) did not reverse aortic dilation and led to aberrant aortic remodeling. An AT2R antagonist, PD123319, reversed the protective effects of losartan in TAC mice. Treatment with compound 21 alone showed no effect on TAC-induced aortic enlargement, blood pressure, elastin breakage, or Mmp9 expression. Conclusions- Our data indicate that when AT1R signaling is blocked, AT2R activation is a key modulator to prevent aortic dilation that occurs with TAC. These data suggest that angiotensin-converting enzyme inhibitor may not be as effective as losartan for slowing aneurysm growth because losartan requires intact AT2R signaling to prevent aortic enlargement.

Published

2019

16. Variants of Unknown Significance in Genes Associated with Heritable Thoracic Aortic Disease Can Be Low Penetrant "Risk Variants".

Author

Kwartler CS, Gong L, Chen J, Wang S, Kulmacz R, Duan XY, Janda A, Huang J, Kamm KE, Stull JT, Guo D, and Milewicz DM

Subjects

Actins genetics, Aortic Dissection genetics, Animals, Disease Models, Animal, Humans, Mice, Aorta, Thoracic pathology, Aortic Aneurysm, Thoracic genetics, Aortic Diseases genetics, Genetic Variation genetics

Abstract

Thoracic aortic aneurysms leading to acute aortic dissections are a preventable cause of premature deaths if individuals at risk can be identified. Individuals with early-onset aortic dissections without a family history or syndromic features have an increased burden of rare genetic variants of unknown significance (VUSs) in genes with pathogenic variants for heritable thoracic aortic disease (HTAD). We assessed the role of VUSs in the development of disease using both in vitro enzymatic assays and mouse models. VUSs in LOX and MYLK identified in individuals with acute aortic dissections were assayed to determine whether they disrupted enzymatic activity. A subset of VUSs reduced enzymatic activity compared to the wild-type proteins but less than pathogenic variants. Additionally, a Myh11 variant, p.Arg247Cys, which does not cause aortic disease in either humans or mice, was crossed with the Acta2 -/- mouse, which has aortic enlargement with age while Acta2 +/- mice do not. Acta2 +/- Myh11 R247C/R247C mice have aortic dilation by 3 months of age without medial degeneration, indicating that two variants not known to cause disease do lead to aortic enlargement in combination. Furthermore, the addition of Myh11 R247C/R247C to the Acta2 -/- mouse model accelerates aortic enlargement and increases medial degeneration. Therefore, our results emphasize the need for a classification system for variants in Mendelian genes that goes beyond the 5-tier system of pathogenic, likely pathogenic, VUS, likely benign, and benign, and includes a designation for low-penetrant "risk variants" that trigger disease either in combination with other risk factors or in a stochastic manner., (Copyright © 2018 American Society of Human Genetics. Published by Elsevier Inc. All rights reserved.)

Published

2018

17. Ari-1 Regulates Myonuclear Organization Together with Parkin and Is Associated with Aortic Aneurysms.

Author

Tan KL, Haelterman NA, Kwartler CS, Regalado ES, Lee PT, Nagarkar-Jaiswal S, Guo DC, Duraine L, Wangler MF, Bamshad MJ, Nickerson DA, Lin G, Milewicz DM, and Bellen HJ

Subjects

Adolescent, Adult, Aged, Aged, 80 and over, Animals, Aortic Aneurysm genetics, Aortic Aneurysm metabolism, Carrier Proteins genetics, Cell Nucleus genetics, Cell Nucleus metabolism, Cell Nucleus pathology, Child, Preschool, Cytoskeleton, Drosophila Proteins genetics, Drosophila melanogaster growth & development, Female, Humans, Male, Middle Aged, Myocytes, Smooth Muscle metabolism, Pedigree, Phenotype, Ubiquitin-Protein Ligases genetics, Young Adult, Aortic Aneurysm pathology, Carrier Proteins metabolism, Drosophila Proteins metabolism, Drosophila melanogaster metabolism, Mutation, Myocytes, Smooth Muscle pathology, Ubiquitin-Protein Ligases metabolism

Abstract

Nuclei are actively positioned and anchored to the cytoskeleton via the LINC (Linker of Nucleoskeleton and Cytoskeleton) complex. We identified mutations in the Parkin-like E3 ubiquitin ligase Ariadne-1 (Ari-1) that affect the localization and distribution of LINC complex members in Drosophila. ari-1 mutants exhibit nuclear clustering and morphology defects in larval muscles. We show that Ari-1 mono-ubiquitinates the core LINC complex member Koi. Surprisingly, we discovered functional redundancy between Parkin and Ari-1: increasing Parkin expression rescues ari-1 mutant phenotypes and vice versa. We further show that rare variants in the human homolog of ari-1 (ARIH1) are associated with thoracic aortic aneurysms and dissections, conditions resulting from smooth muscle cell (SMC) dysfunction. Human ARIH1 rescues fly ari-1 mutant phenotypes, whereas human variants found in patients fail to do so. In addition, SMCs obtained from patients display aberrant nuclear morphology. Hence, ARIH1 is critical in anchoring myonuclei to the cytoskeleton., (Copyright © 2018 Elsevier Inc. All rights reserved.)

Published

2018

18. Loss of Smooth Muscle α-Actin Leads to NF-κB-Dependent Increased Sensitivity to Angiotensin II in Smooth Muscle Cells and Aortic Enlargement.

Author

Chen J, Peters A, Papke CL, Villamizar C, Ringuette LJ, Cao J, Wang S, Ma S, Gong L, Byanova KL, Xiong J, Zhu MX, Madonna R, Kee P, Geng YJ, Brasier AR, Davis EC, Prakash S, Kwartler CS, and Milewicz DM

Subjects

Actins drug effects, Actins genetics, Angiotensin II Type 1 Receptor Blockers pharmacology, Animals, Aorta, Thoracic drug effects, Aorta, Thoracic pathology, Cells, Cultured, Mice, Mice, 129 Strain, Mice, Inbred C57BL, Mice, Knockout, Muscle, Smooth, Vascular drug effects, Muscle, Smooth, Vascular metabolism, Myocytes, Smooth Muscle drug effects, Random Allocation, Reactive Oxygen Species metabolism, Receptor, Angiotensin, Type 1 genetics, Actins deficiency, Angiotensin II metabolism, Aorta, Thoracic metabolism, Myocytes, Smooth Muscle metabolism, NF-kappa B metabolism, Receptor, Angiotensin, Type 1 biosynthesis

Abstract

Rationale: Mutations in ACTA2 , encoding the smooth muscle isoform of α-actin, cause thoracic aortic aneurysms, acute aortic dissections, and occlusive vascular diseases., Objective: We sought to identify the mechanism by which loss of smooth muscle α-actin causes aortic disease., Methods and Results: Acta2 -/- mice have an increased number of elastic lamellae in the ascending aorta and progressive aortic root dilation as assessed by echocardiography that can be attenuated by treatment with losartan, an angiotensin II (AngII) type 1 receptor blocker. AngII levels are not increased in Acta2 -/- aortas or kidneys. Aortic tissue and explanted smooth muscle cells from Acta2 -/- aortas show increased production of reactive oxygen species and increased basal nuclear factor κB signaling, leading to an increase in the expression of the AngII receptor type I a and activation of signaling at 100-fold lower levels of AngII in the mutant compared with wild-type cells. Furthermore, disruption of smooth muscle α-actin filaments in wild-type smooth muscle cells by various mechanisms activates nuclear factor κB signaling and increases expression of AngII receptor type I a., Conclusions: These findings reveal that disruption of smooth muscle α-actin filaments in smooth muscle cells increases reactive oxygen species levels, activates nuclear factor κB signaling, and increases AngII receptor type I a expression, thus potentiating AngII signaling in vascular smooth muscle cells without an increase in the exogenous levels of AngII., (© 2017 American Heart Association, Inc.)

Published

2017

19. Loss-of-Function Mutations in YY1AP1 Lead to Grange Syndrome and a Fibromuscular Dysplasia-Like Vascular Disease.

Author

Guo DC, Duan XY, Regalado ES, Mellor-Crummey L, Kwartler CS, Kim D, Lieberman K, de Vries BBA, Pfundt R, Schinzel A, Kotzot D, Shen X, Yang ML, Bamshad MJ, Nickerson DA, Gornik HL, Ganesh SK, Braverman AC, Grange DK, and Milewicz DM

Subjects

Adolescent, Adult, Bone and Bones pathology, Brachydactyly genetics, Cell Cycle Checkpoints genetics, Cell Cycle Proteins, Exome genetics, Female, Genes, Recessive, Heterozygote, Homozygote, Humans, Learning Disabilities genetics, Male, Middle Aged, Pedigree, Syndactyly genetics, Syndrome, Fibromuscular Dysplasia genetics, Muscle, Smooth, Vascular metabolism, Muscle, Smooth, Vascular pathology, Mutation, Nuclear Proteins genetics, Transcription Factors genetics

Abstract

Fibromuscular dysplasia (FMD) is a heterogeneous group of non-atherosclerotic and non-inflammatory arterial diseases that primarily involves the renal and cerebrovascular arteries. Grange syndrome is an autosomal-recessive condition characterized by severe and early-onset vascular disease similar to FMD and variable penetrance of brachydactyly, syndactyly, bone fragility, and learning disabilities. Exome-sequencing analysis of DNA from three affected siblings with Grange syndrome identified compound heterozygous nonsense variants in YY1AP1, and homozygous nonsense or frameshift YY1AP1 variants were subsequently identified in additional unrelated probands with Grange syndrome. YY1AP1 encodes yin yang 1 (YY1)-associated protein 1 and is an activator of the YY1 transcription factor. We determined that YY1AP1 localizes to the nucleus and is a component of the INO80 chromatin remodeling complex, which is responsible for transcriptional regulation, DNA repair, and replication. Molecular studies revealed that loss of YY1AP1 in vascular smooth muscle cells leads to cell cycle arrest with decreased proliferation and increased levels of the cell cycle regulator p21/WAF/CDKN1A and disrupts TGF-β-driven differentiation of smooth muscle cells. Identification of YY1AP1 mutations as a cause of FMD indicates that this condition can result from underlying genetic variants that significantly alter the phenotype of vascular smooth muscle cells., (Copyright © 2017 American Society of Human Genetics. Published by Elsevier Inc. All rights reserved.)

Published

2017

20. FOXE3 mutations predispose to thoracic aortic aneurysms and dissections.

Author

Kuang SQ, Medina-Martinez O, Guo DC, Gong L, Regalado ES, Reynolds CL, Boileau C, Jondeau G, Prakash SK, Kwartler CS, Zhu LY, Peters AM, Duan XY, Bamshad MJ, Shendure J, Nickerson DA, Santos-Cortez RL, Dong X, Leal SM, Majesky MW, Swindell EC, Jamrich M, and Milewicz DM

Subjects

Adult, Aortic Dissection metabolism, Aortic Dissection pathology, Animals, Aorta metabolism, Aorta pathology, Aortic Aneurysm, Thoracic metabolism, Aortic Aneurysm, Thoracic pathology, Apoptosis, Cells, Cultured, Cyclin-Dependent Kinase Inhibitor p21 metabolism, Female, Gene Expression, Genetic Association Studies, Genetic Predisposition to Disease, Humans, Male, Mice, Inbred C57BL, Mice, Knockout, Middle Aged, Muscle, Smooth, Vascular pathology, Mutation, Missense, Myocytes, Smooth Muscle physiology, Pedigree, Tumor Suppressor Protein p53 genetics, Vascular Remodeling, Zebrafish, Aortic Dissection genetics, Aortic Aneurysm, Thoracic genetics, Forkhead Transcription Factors genetics

Abstract

The ascending thoracic aorta is designed to withstand biomechanical forces from pulsatile blood. Thoracic aortic aneurysms and acute aortic dissections (TAADs) occur as a result of genetically triggered defects in aortic structure and a dysfunctional response to these forces. Here, we describe mutations in the forkhead transcription factor FOXE3 that predispose mutation-bearing individuals to TAAD. We performed exome sequencing of a large family with multiple members with TAADs and identified a rare variant in FOXE3 with an altered amino acid in the DNA-binding domain (p.Asp153His) that segregated with disease in this family. Additional pathogenic FOXE3 variants were identified in unrelated TAAD families. In mice, Foxe3 deficiency reduced smooth muscle cell (SMC) density and impaired SMC differentiation in the ascending aorta. Foxe3 expression was induced in aortic SMCs after transverse aortic constriction, and Foxe3 deficiency increased SMC apoptosis and ascending aortic rupture with increased aortic pressure. These phenotypes were rescued by inhibiting p53 activity, either by administration of a p53 inhibitor (pifithrin-α), or by crossing Foxe3-/- mice with p53-/- mice. Our data demonstrate that FOXE3 mutations lead to a reduced number of aortic SMCs during development and increased SMC apoptosis in the ascending aorta in response to increased biomechanical forces, thus defining an additional molecular pathway that leads to familial thoracic aortic disease.

Published

2016

21. Overexpression of smooth muscle myosin heavy chain leads to activation of the unfolded protein response and autophagic turnover of thick filament-associated proteins in vascular smooth muscle cells.

Author

Kwartler CS, Chen J, Thakur D, Li S, Baskin K, Wang S, Wang ZV, Walker L, Hill JA, Epstein HF, Taegtmeyer H, and Milewicz DM

Subjects

Animals, Calcium Signaling, Chromosome Duplication, Chromosomes, Human, Pair 16 genetics, Endoplasmic Reticulum Stress, Gene Expression, Humans, Mice, Muscle Contraction, Muscle, Smooth, Vascular physiology, Autophagy, Muscle, Smooth, Vascular cytology, Muscle, Smooth, Vascular metabolism, Myosin Heavy Chains genetics, Myosin Heavy Chains metabolism, Unfolded Protein Response

Abstract

Duplications spanning nine genes at the genomic locus 16p13.1 predispose individuals to acute aortic dissections. The most likely candidate gene in this region leading to the predisposition for dissection is MYH11, which encodes smooth muscle myosin heavy chain (SM-MHC). The effects of increased expression of MYH11 on smooth muscle cell (SMC) phenotypes were explored using mouse aortic SMCs with transgenic overexpression of one isoform of SM-MHC. We found that these cells show increased expression of Myh11 and myosin filament-associated contractile genes at the message level when compared with control SMCs, but not at the protein level due to increased protein degradation. Increased expression of Myh11 resulted in endoplasmic reticulum (ER) stress in SMCs, which led to a paradoxical decrease of protein levels through increased autophagic degradation. An additional consequence of ER stress in SMCs was increased intracellular calcium ion concentration, resulting in increased contractile signaling and contraction. The increased signals for contraction further promote transcription of contractile genes, leading to a feedback loop of metabolic abnormalities in these SMCs. We suggest that overexpression of MYH11 can lead to increased ER stress and autophagy, findings that may be globally implicated in disease processes associated with genomic duplications., (© 2014 by The American Society for Biochemistry and Molecular Biology, Inc.)

Published

2014

22. Aortic remodeling after transverse aortic constriction in mice is attenuated with AT1 receptor blockade.

Author

Kuang SQ, Geng L, Prakash SK, Cao JM, Guo S, Villamizar C, Kwartler CS, Peters AM, Brasier AR, and Milewicz DM

Subjects

Animals, Aorta metabolism, Aorta pathology, Aorta physiopathology, Aorta surgery, Aortic Aneurysm, Thoracic etiology, Aortic Aneurysm, Thoracic metabolism, Aortic Aneurysm, Thoracic pathology, Aortic Aneurysm, Thoracic physiopathology, Arterial Pressure, Biomechanical Phenomena, Collagen metabolism, Constriction, Dilatation, Pathologic, Disease Models, Animal, Echocardiography, Doppler, Hypertension complications, Hypertension metabolism, Hypertension pathology, Hypertension physiopathology, Male, Mice, Mice, Inbred C57BL, Receptor, Angiotensin, Type 1 metabolism, Smad2 Protein metabolism, Time Factors, Transforming Growth Factor beta1 metabolism, Angiotensin II Type 1 Receptor Blockers pharmacology, Antihypertensive Agents pharmacology, Aorta drug effects, Aortic Aneurysm, Thoracic prevention & control, Hypertension drug therapy, Losartan pharmacology, Receptor, Angiotensin, Type 1 drug effects

Abstract

Objective: Although hypertension is the most common risk factor for thoracic aortic diseases, it is not understood how increased pressures on the ascending aorta lead to aortic aneurysms. We investigated the role of angiotensin II type 1 receptor activation in ascending aortic remodeling in response to increased biomechanical forces using a transverse aortic constriction (TAC) mouse model., Approach and Results: Two weeks after TAC, the increased biomechanical pressures led to ascending aortic dilatation and thickening of the medial and adventitial layers of the aorta. There was significant adventitial hyperplasia and inflammatory responses in TAC ascending aortas were accompanied by increased adventitial collagen, elevated inflammatory and proliferative markers, and increased cell density attributable to accumulation of myofibroblasts and macrophages. Treatment with losartan significantly blocked TAC-induced vascular inflammation and macrophage accumulation. However, losartan only partially prevented TAC-induced adventitial hyperplasia, collagen accumulation, and ascending aortic dilatation. Increased Tgfb2 expression and phosphorylated-Smad2 staining in the medial layer of TAC ascending aortas were effectively blocked with losartan. In contrast, the increased Tgfb1 expression and adventitial phospho-Smad2 staining were only partially attenuated by losartan. In addition, losartan significantly blocked extracellular signal-regulated kinase activation and reactive oxygen species production in the TAC ascending aorta., Conclusions: Inhibition of the angiotensin II type 1 receptor using losartan significantly attenuated the vascular remodeling associated with TAC but did not completely block the increased transforming growth factor-β1 expression, adventitial Smad2 signaling, and collagen accumulation. These results help to delineate the aortic transforming growth factor-β signaling that is dependent and independent of the angiotensin II type 1 receptor after TAC.

Published

2013

23. Smooth muscle hyperplasia due to loss of smooth muscle α-actin is driven by activation of focal adhesion kinase, altered p53 localization and increased levels of platelet-derived growth factor receptor-β.

Author

Papke CL, Cao J, Kwartler CS, Villamizar C, Byanova KL, Lim SM, Sreenivasappa H, Fischer G, Pham J, Rees M, Wang M, Chaponnier C, Gabbiani G, Khakoo AY, Chandra J, Trache A, Zimmer W, and Milewicz DM

Subjects

Actins genetics, Animals, Cell Movement genetics, Cell Nucleus metabolism, Cell Proliferation, Enzyme Activation, Hyperplasia, Mice, Mice, Knockout, Models, Biological, Phenotype, Protein Transport, Reactive Oxygen Species metabolism, Actins metabolism, Focal Adhesion Protein-Tyrosine Kinases metabolism, Myocytes, Smooth Muscle metabolism, Myocytes, Smooth Muscle pathology, Receptor, Platelet-Derived Growth Factor beta metabolism, Tumor Suppressor Protein p53 metabolism

Abstract

Mutations in ACTA2, encoding the smooth muscle cell (SMC)-specific isoform of α-actin (α-SMA), cause thoracic aortic aneurysms and dissections and occlusive vascular diseases, including early onset coronary artery disease and stroke. We have shown that occlusive arterial lesions in patients with heterozygous ACTA2 missense mutations show increased numbers of medial or neointimal SMCs. The contribution of SMC hyperplasia to these vascular diseases and the pathways responsible for linking disruption of α-SMA filaments to hyperplasia are unknown. Here, we show that the loss of Acta2 in mice recapitulates the SMC hyperplasia observed in ACTA2 mutant SMCs and determine the cellular pathways responsible for SMC hyperplasia. Acta2(-/-) mice showed increased neointimal formation following vascular injury in vivo, and SMCs explanted from these mice demonstrated increased proliferation and migration. Loss of α-SMA induced hyperplasia through focal adhesion (FA) rearrangement, FA kinase activation, re-localization of p53 from the nucleus to the cytoplasm and increased expression and ligand-independent activation of platelet-derived growth factor receptor beta (Pdgfr-β). Disruption of α-SMA in wild-type SMCs also induced similar cellular changes. Imatinib mesylate inhibited Pdgfr-β activation and Acta2(-/-) SMC proliferation in vitro and neointimal formation with vascular injury in vivo. Loss of α-SMA leads to SMC hyperplasia in vivo and in vitro through a mechanism involving FAK, p53 and Pdgfr-β, supporting the hypothesis that SMC hyperplasia contributes to occlusive lesions in patients with ACTA2 missense mutations.

Published

2013

24. TGFB2 mutations cause familial thoracic aortic aneurysms and dissections associated with mild systemic features of Marfan syndrome.

Author

Boileau C, Guo DC, Hanna N, Regalado ES, Detaint D, Gong L, Varret M, Prakash SK, Li AH, d'Indy H, Braverman AC, Grandchamp B, Kwartler CS, Gouya L, Santos-Cortez RL, Abifadel M, Leal SM, Muti C, Shendure J, Gross MS, Rieder MJ, Vahanian A, Nickerson DA, Michel JB, Jondeau G, and Milewicz DM

Subjects

Aortic Dissection metabolism, Aortic Dissection pathology, Aortic Aneurysm, Thoracic metabolism, Aortic Aneurysm, Thoracic pathology, Codon, Nonsense, Exome, Female, Frameshift Mutation, Genetic Predisposition to Disease, Genome-Wide Association Study, Haploinsufficiency, Humans, Lod Score, Male, Pedigree, Transforming Growth Factor beta2 metabolism, Aortic Dissection genetics, Aortic Aneurysm, Thoracic genetics, Marfan Syndrome genetics, Mutation, Transforming Growth Factor beta2 genetics

Abstract

A predisposition for thoracic aortic aneurysms leading to acute aortic dissections can be inherited in families in an autosomal dominant manner. Genome-wide linkage analysis of two large unrelated families with thoracic aortic disease followed by whole-exome sequencing of affected relatives identified causative mutations in TGFB2. These mutations-a frameshift mutation in exon 6 and a nonsense mutation in exon 4-segregated with disease with a combined logarithm of odds (LOD) score of 7.7. Sanger sequencing of 276 probands from families with inherited thoracic aortic disease identified 2 additional TGFB2 mutations. TGFB2 encodes transforming growth factor (TGF)-β2, and the mutations are predicted to cause haploinsufficiency for TGFB2; however, aortic tissue from cases paradoxically shows increased TGF-β2 expression and immunostaining. Thus, haploinsufficiency for TGFB2 predisposes to thoracic aortic disease, suggesting that the initial pathway driving disease is decreased cellular TGF-β2 levels leading to a secondary increase in TGF-β2 production in the diseased aorta.

Published

2012

25. Rare, nonsynonymous variant in the smooth muscle-specific isoform of myosin heavy chain, MYH11, R247C, alters force generation in the aorta and phenotype of smooth muscle cells.

Author

Kuang SQ, Kwartler CS, Byanova KL, Pham J, Gong L, Prakash SK, Huang J, Kamm KE, Stull JT, Sweeney HL, and Milewicz DM

Subjects

Adenosine Triphosphate metabolism, Animals, Aorta metabolism, Binding Sites, Carotid Arteries metabolism, Carotid Arteries pathology, Carotid Artery Injuries genetics, Carotid Artery Injuries metabolism, Carotid Artery Injuries pathology, Cell Differentiation, Cell Proliferation, Cells, Cultured, Disease Models, Animal, Focal Adhesions metabolism, Focal Adhesions pathology, Gene Knock-In Techniques, Genotype, Kinetics, Mice, Mice, 129 Strain, Mice, Inbred C57BL, Mice, Transgenic, Myosin Heavy Chains genetics, Phenotype, Trans-Activators metabolism, Transfection, rho GTP-Binding Proteins metabolism, Muscle, Smooth, Vascular metabolism, Mutation, Myocytes, Smooth Muscle metabolism, Myosin Heavy Chains metabolism, Vasoconstriction genetics

Abstract

Rationale: Mutations in myosin heavy chain (MYH11) cause autosomal dominant inheritance of thoracic aortic aneurysms and dissections. At the same time, rare, nonsynonymous variants in MYH11 that are predicted to disrupt protein function but do not cause inherited aortic disease are common in the general population and the vascular disease risk associated with these variants is unknown., Objective: To determine the consequences of the recurrent MYH11 rare variant, R247C, through functional studies in vitro and analysis of a knock-in mouse model with this specific variant, including assessment of aortic contraction, response to vascular injury, and phenotype of primary aortic smooth muscle cells (SMCs)., Methods and Results: The steady state ATPase activity (actin-activated) and the rates of phosphate and ADP release were lower for the R247C mutant myosin than for the wild-type, as was the rate of actin filament sliding in an in vitro motility assay. Myh11(R247C/R247C) mice exhibited normal growth, reproduction, and aortic histology but decreased aortic contraction. In response to vascular injury, Myh11(R247C/R247C) mice showed significantly increased neointimal formation due to increased SMC proliferation when compared with the wild-type mice. Primary aortic SMCs explanted from the Myh11(R247C/R247C) mice were dedifferentiated compared with wild-type SMCs based on increased proliferation and reduced expression of SMC contractile proteins. The mutant SMCs also displayed altered focal adhesions and decreased Rho activation, associated with decreased nuclear localization of myocardin-related transcription factor-A. Exposure of the Myh11(R247C/R247C) SMCs to a Rho activator rescued the dedifferentiated phenotype of the SMCs., Conclusions: These results indicate that a rare variant in MYH11, R247C, alters myosin contractile function and SMC phenotype, leading to increased proliferation in vitro and in response to vascular injury.

Published

2012

26. Notch signaling is antagonized by SAO-1, a novel GYF-domain protein that interacts with the E3 ubiquitin ligase SEL-10 in Caenorhabditis elegans.

Author

Hale VA, Guiney EL, Goldberg LY, Haduong JH, Kwartler CS, Scangos KW, and Goutte C

Subjects

Adaptor Proteins, Signal Transducing, Amino Acid Sequence, Animals, Caenorhabditis elegans embryology, Caenorhabditis elegans genetics, Caenorhabditis elegans Proteins chemistry, Carrier Proteins chemistry, DNA-Binding Proteins genetics, DNA-Binding Proteins metabolism, Embryonic Development genetics, Gene Order, Genes, Lethal, Glucagon-Like Peptide-1 Receptor, Homeodomain Proteins genetics, Homeodomain Proteins metabolism, Molecular Sequence Data, Mutation, Protein Binding, Protein Structure, Tertiary, Receptors, Glucagon genetics, Receptors, Glucagon metabolism, Receptors, Notch antagonists & inhibitors, Sequence Alignment, Signal Transduction, Caenorhabditis elegans metabolism, Caenorhabditis elegans Proteins genetics, Caenorhabditis elegans Proteins metabolism, Carrier Proteins genetics, Carrier Proteins metabolism, Cell Cycle Proteins metabolism, Receptors, Notch metabolism, Ubiquitin-Protein Ligases metabolism

Abstract

Notch signaling pathways can be regulated through a variety of cellular mechanisms, and genetically compromised systems provide useful platforms from which to search for the responsible modulators. The Caenorhabditis elegans gene aph-1 encodes a component of γ-secretase, which is essential for Notch signaling events throughout development. By looking for suppressors of the incompletely penetrant aph-1(zu147) mutation, we identify a new gene, sao-1 (suppressor of aph-one), that negatively regulates aph-1(zu147) activity in the early embryo. The sao-1 gene encodes a novel protein that contains a GYF protein-protein interaction domain and interacts specifically with SEL-10, an Fbw7 component of SCF E3 ubiquitin ligases. We demonstrate that the embryonic lethality of aph-1(zu147) mutants can be suppressed by removing sao-1 activity or by mutations that disrupt the SAO-1-SEL-10 protein interaction. Decreased sao-1 activity also influences Notch signaling events when they are compromised at different molecular steps of the pathway, such as at the level of the Notch receptor GLP-1 or the downstream transcription factor LAG-1. Combined analysis of the SAO-1-SEL-10 protein interaction and comparisons of sao-1 and sel-10 genetic interactions suggest a possible role for SAO-1 as an accessory protein that participates with SEL-10 in downregulation of Notch signaling. This work provides the first mutant analysis of a GYF-domain protein in either C. elegans or Drosophila and introduces a new type of Fbw7-interacting protein that acts in a subset of Fbw7 functions.

Published

2012

27. TGFBR2 mutations alter smooth muscle cell phenotype and predispose to thoracic aortic aneurysms and dissections.

Author

Inamoto S, Kwartler CS, Lafont AL, Liang YY, Fadulu VT, Duraisamy S, Willing M, Estrera A, Safi H, Hannibal MC, Carey J, Wiktorowicz J, Tan FK, Feng XH, Pannu H, and Milewicz DM

Subjects

Actins metabolism, Aortic Dissection metabolism, Animals, Aortic Aneurysm, Thoracic metabolism, Calcium-Binding Proteins metabolism, Calmodulin-Binding Proteins metabolism, Case-Control Studies, Cell Differentiation drug effects, Cell Differentiation physiology, Cell Line, Cell Proliferation, Cells, Cultured, Humans, Mice, Microfilament Proteins metabolism, Muscle, Smooth, Vascular drug effects, Muscle, Smooth, Vascular metabolism, Myofibroblasts metabolism, Phenotype, Protein Serine-Threonine Kinases metabolism, Receptor, Transforming Growth Factor-beta Type II, Receptors, Transforming Growth Factor beta metabolism, Signal Transduction physiology, Transfection, Transforming Growth Factor beta1 pharmacology, Calponins, Aortic Dissection genetics, Aortic Aneurysm, Thoracic genetics, Cell Differentiation genetics, Genetic Predisposition to Disease genetics, Muscle, Smooth, Vascular cytology, Myofibroblasts cytology, Protein Serine-Threonine Kinases genetics, Receptors, Transforming Growth Factor beta genetics

Abstract

Aims: Transforming growth factor-β (TGF-β) signaling is critical for the differentiation of smooth muscle cells (SMCs) into quiescent cells expressing a full repertoire of contractile proteins. Heterozygous mutations in TGF-β receptor type II (TGFBR2) disrupt TGF-β signaling and lead to genetic conditions that predispose to thoracic aortic aneurysms and dissections (TAADs). The aim of this study is to determine the molecular mechanism by which TGFBR2 mutations cause TAADs., Methods and Results: Using aortic SMCs explanted from patients with TGFBR2 mutations, we show decreased expression of SMC contractile proteins compared with controls. Exposure to TGF-β1 fails to increase expression of contractile genes in mutant SMCs, whereas control cells further increase expression of these genes. Analysis of fixed and frozen aortas from patients with TGFBR2 mutations confirms decreased in vivo expression of contractile proteins relative to unaffected aortas. Fibroblasts explanted from patients with TGFBR2 mutations fail to transform into mature myofibroblasts with TGF-β1 stimulation as assessed by expression of contractile proteins., Conclusions: These data support the conclusion that heterozygous TGFBR2 mutations lead to decreased expression of SMC contractile protein in both SMCs and myofibroblasts. The failure of TGFBR2-mutant SMCs to fully express SMC contractile proteins predicts defective contractile function in these cells and aligns with a hypothesis that defective SMC contractile function contributes to the pathogenesis of TAAD.

Published

2010

28. Thoracic aortic disease in tuberous sclerosis complex: molecular pathogenesis and potential therapies in Tsc2+/- mice.

Author

Cao J, Gong L, Guo DC, Mietzsch U, Kuang SQ, Kwartler CS, Safi H, Estrera A, Gambello MJ, and Milewicz DM

Subjects

Animals, Aorta, Thoracic diagnostic imaging, Aorta, Thoracic drug effects, Aorta, Thoracic metabolism, Aortic Aneurysm metabolism, Aortic Aneurysm pathology, Cell Proliferation drug effects, Child, Contractile Proteins metabolism, Elastin pharmacology, Humans, Magnetic Resonance Angiography, Mechanistic Target of Rapamycin Complex 1, Mice, Multiprotein Complexes, Mutation genetics, Myocytes, Smooth Muscle drug effects, Myocytes, Smooth Muscle metabolism, Myocytes, Smooth Muscle pathology, Peptides pharmacology, Phenotype, Proteins, Radiography, Signal Transduction drug effects, TOR Serine-Threonine Kinases, Thoracic Diseases diagnosis, Transcription Factors metabolism, Tuberous Sclerosis Complex 2 Protein, Tumor Suppressor Proteins metabolism, Tunica Intima drug effects, Tunica Intima metabolism, Tunica Intima pathology, rho GTP-Binding Proteins metabolism, Aorta, Thoracic pathology, Thoracic Diseases genetics, Thoracic Diseases therapy, Tumor Suppressor Proteins deficiency

Abstract

Tuberous sclerosis complex (TSC) is a genetic disorder with pleiotropic manifestations caused by heterozygous mutations in either TSC1 or TSC2. One of the less investigated complications of TSC is the formation of aneurysms of the descending aorta, which are characterized on pathologic examination by smooth muscle cell (SMC) proliferation in the aortic media. SMCs were explanted from Tsc2(+/-) mice to investigate the pathogenesis of aortic aneurysms caused by TSC2 mutations. Tsc2(+/-) SMCs demonstrated increased phosphorylation of mammalian target of rapamycin (mTOR), S6 and p70S6K and increased proliferation rates compared with wild-type (WT) SMCs. Tsc2(+/-) SMCs also had reduced expression of SMC contractile proteins compared with WT SMCs. An inhibitor of mTOR signaling, rapamycin, decreased SMC proliferation and increased contractile protein expression in the Tsc2(+/-) SMCs to levels similar to WT SMCs. Exposure to alpha-elastin fragments also decreased proliferation of Tsc2(+/-) SMCs and increased levels of p27(kip1), but failed to increase expression of contractile proteins. In response to artery injury using a carotid artery ligation model, Tsc2(+/-) mice significantly increased neointima formation compared with the control mice, and the neointima formation was inhibited by treatment with rapamycin. These results demonstrate that Tsc2 haploinsufficiency in SMCs increases proliferation and decreases contractile protein expression and suggest that the increased proliferative potential of the mutant cells may be suppressed in vivo by interaction with elastin. These findings provide insights into the molecular pathogenesis of aortic disease in TSC patients and identify a potential therapeutic target for treatment of this complication of the disease.

Published

2010

29. Genetic variants promoting smooth muscle cell proliferation can result in diffuse and diverse vascular diseases: evidence for a hyperplastic vasculomyopathy.

Author

Milewicz DM, Kwartler CS, Papke CL, Regalado ES, Cao J, and Reid AJ

Subjects

Actins genetics, Adult, Coronary Vessels metabolism, Coronary Vessels pathology, Humans, Hyperplasia, Myocytes, Smooth Muscle pathology, Neurofibromin 1 genetics, Vascular Diseases pathology, Cell Proliferation, Mutation, Myocytes, Smooth Muscle metabolism, Vascular Diseases genetics

Abstract

Genetic predisposition to early onset of occlusive vascular diseases, including coronary artery disease, ischemic stroke, and Moyamoya disease, may represent varying presentations of a common underlying dysregulation of vascular smooth muscle cell proliferation. We discuss mutations in two genes, NF1 and ACTA2, which predispose affected individuals to diffuse and diverse vascular diseases. These patients show evidence of diffuse occlusive disease in multiple arterial beds or even develop seemingly diverse arterial pathologies, ranging from occlusions to arterial aneurysms. We also present the current evidence that both NF1 and ACTA2 mutations promote increased smooth muscle cell proliferation in vitro and in vivo, which leads us to propose that these diffuse and diverse vascular diseases are the outward signs of a more fundamental disease: a hyperplastic vasculomyopathy. We suggest that the concept of a hyperplastic vasculomyopathy offers a new approach not only to identifying mutated genes that lead to vascular diseases but also to counseling and possibly treating patients harboring such mutations. In other words, this framework may offer the opportunity to therapeutically target the inappropriate smooth muscle cell behavior that predisposes to a variety of vascular diseases throughout the arterial system.

Published

2010

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

Author

Milewicz DM, Guo DC, Tran-Fadulu V, Lafont AL, Papke CL, Inamoto S, Kwartler CS, and Pannu H

Subjects

Aortic Dissection etiology, Aortic Dissection physiopathology, Aortic Dissection therapy, Animals, Aortic Aneurysm, Thoracic etiology, Aortic Aneurysm, Thoracic physiopathology, Aortic Aneurysm, Thoracic therapy, Female, Humans, Male, Models, Genetic, Muscle Contraction genetics, Muscle, Smooth, Vascular physiopathology, Mutation, Pedigree, Syndrome, Aortic Dissection genetics, Aortic Aneurysm, Thoracic genetics

Abstract

Thoracic aortic aneurysms leading to type A dissections (TAAD) can be inherited in isolation or in association with genetic syndromes, such as Marfan syndrome and Loeys-Dietz syndrome. When TAAD occurs in the absence of syndromic features, it is inherited in an autosomal dominant manner with decreased penetrance and variable expression, the disease is referred to as familial TAAD. Familial TAAD exhibits significant clinical and genetic heterogeneity. The first genes identified to cause TAAD were FBN1, TGFBR2, and TGFBR1. The identification and characterization of these genes suggested that increased TGF-beta signaling plays a role in pathogenesis. The recent discovery that mutations in the vascular smooth muscle cell (SMC)-specific beta-myosin (MYH11) and alpha-actin (ACTA2) can also cause this disorder has focused attention on the importance of the maintenance of SMC contractile function in preserving aortic structure and preventing TAAD.

Published

2008