Novel Mutations in BMPR2, ACVRL1 and KCNA5 Genes and Hemodynamic Parameters in Patients with Pulmonary Arterial Hypertension

Pousada, Guillermo; Baloira, Adolfo; Vilariño, Carlos; Cifrián, José; Valverde, Diana

doi:10.1371/journal.pone.0100261

Cited by 45 publications

(55 citation statements)

References 42 publications

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“…10, 22, 23 . In summary, 55 unrelated PAH patients of Spanish origin (28 IPAH, 18 APAH associated to connective tissue disease, 4 related to HIV and 5 porto-pulmonary hypertension) (Fig.…”

Section: Resultsmentioning

confidence: 99%

Molecular and functional characterization of the BMPR2 gene in Pulmonary Arterial Hypertension

Pousada

Lupo

Castro-Sánchez

et al. 2017

Sci Rep

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Pulmonary arterial hypertension is a progressive disease that causes the obstruction of precapillary pulmonary arteries and a sustained increase in pulmonary vascular resistance. The aim was to analyze functionally the variants found in the BMPR2 gene and to establish a genotype-phenotype correlation. mRNA expression studies were performed using pSPL3 vector, studies of subcellular localization were performed using pEGFP-N1 vector and luciferase assays were performed using pGL3-Basic vector. We have identified 30 variants in the BMPR2 gene in 27 of 55 patients. In 16 patients we detected pathogenic mutations. Minigene assays revealed that 6 variants (synonymous, missense) result in splicing defect. By immunofluorescence assay, we observed that 4 mutations affect the protein localization. Finally, 4 mutations located in the 5′UTR region showed a decreased transcriptional activity in luciferase assays. Genotype-phenotype correlation, revealed that patients with pathogenic mutations have a more severe phenotype (sPaP p = 0.042, 6MWT p = 0.041), a lower age at diagnosis (p = 0.040) and seemed to have worse response to phosphodiesterase-5-inhibitors (p = 0.010). Our study confirms that in vitro expression analysis is a suitable approach in order to investigate the phenotypic consequences of the nucleotide variants, especially in cases where the involved genes have a pattern of expression in tissues of difficult access.

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“…10, 22, 23 . In summary, 55 unrelated PAH patients of Spanish origin (28 IPAH, 18 APAH associated to connective tissue disease, 4 related to HIV and 5 porto-pulmonary hypertension) (Fig.…”

Section: Resultsmentioning

confidence: 99%

Molecular and functional characterization of the BMPR2 gene in Pulmonary Arterial Hypertension

Pousada

Lupo

Castro-Sánchez

et al. 2017

Sci Rep

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“…The Smad dimer then enters the nucleus where it acts as a transcription factor, regulating the transcription of angiogenesis genes such as VEGF. Reduced presence of endoglin, a coreceptor for ALK family of receptors, has been shown to decrease the activity of the ALK1 pathway, as well as the ALK5 pathway that counterbalances ALK1 activity by promoting cell c.24A > T Missense p.Lys8Ans [16] c.31_50del20 Deletion p.Leu11Glyfs*20 [17] c.37delC Deletion p.Leu13Cysfs*2 [18] c.50dupT Duplication p.Leu17Phefs*21 [19] c.50_53delTGGT Deletion p.Leu*17 [20] c.61 + 1G > A Missense p.? [14] c.61 + 10G > A Splice Site p.?…”

Section: Discussionmentioning

confidence: 99%

“…[39] c.626-3C > G Splice Site p.? [55] c.632G > A Missense p.Gly211Asp [51] c.639T > G Missense p.Tyr213* [14] c.641delG Deletion p.Gly214Alafs*44 [45] c.643G > A Missense p.Glu215Lys [31] c.647T > G Missense p.Val216Gly [19] c.649T > G Missense p.Trp217Gly [45] c.650G > A Missense p.Trp217* [20] c.651G > A Missense p.Trp217* [24] c.653_654delGGinsCC Delins p.Arg218Pro [52] c.656G > A Missense p.Gly219Asp [24] c.661T > G Missense p.Trp221Gly [14] c.662G > A Missense p.Trp221* [19] c.663G > A Missense p.Trp221* [47] c.664_668delCACGG Deletion p.His222* [31] Continued c.667G > C Missense p.Gly223Arg [31] c.670G > A Missense p.Glu224Lys [25] c.673A > T Missense p.Ser225Cys [16] c.673_674delAG Deletion p.Ser225Cysfs*11 [47] c.676G > C Missense p.Val226Leu [30] c.677T > A Missense p.Val226Glu [45] c.682delG Deletion p.Val228Serfs*30 [31] c.683T > A Missense p.Val228Asp [19] c.686A > T Missense p.Lys229Met [55] c.686A > G Missense p.Lys229Arg [31] c.696_698delCTC Deletion p.Ser233del [56] c.698C > T Missense p.Ser233Leu [37] c.698C > A Missense p.Ser233* [57] c.704delA Deletion p.Asp235Valfs*23 [31] c.709C > T Missense p.Gln237* [25] c.716G > A Missense p.Trp239* [46] c.743_744delCA Deletion p.Thr248Serfs*143 [29] c.760_762delGAC Deletion p.Asp254del [18] c.759_761delCGA Deletion p.Asp254del [31] c.772 + 3_772 + 4dupAA Duplication p.? [43] c.772 + 5G > A Missense p.?…”

Section: Discussionmentioning

confidence: 99%

Novel ACLV1 Mutation Identified in Late Onset Hereditary Hemorrhagic Telangiectasia

Patrick¹,

McIntyre²,

Ramidial³

et al. 2016

IJOHNS

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“…45 Patients carrying a mutation in the BMPR2, ALK1 and KCNA5 genes had a higher value of mean pulmonary pressure and pulmonary vascular resistance, and a significantly lower cardiac index than non-carriers. 47 An imbalance of increased TGF-b levels and decreased BMP signals induced by BMPR2 mutations leads to PAH. 48 The p.(S225C) mutation is located in exon 6 of ALK1 gene and it is placed in the serineethreonine kinase domain.…”

Section: Clinical Significancementioning

confidence: 99%

Pulmonary artery hypertension in childhood: The transforming growth factor-β superfamily-related genes

Yuan

2018

Pediatrics & Neonatology

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Pulmonary artery hypertension (PAH) is very rare in childhood, and it can be divided into heritable, idiopathic drug- and toxin-induced and other disease (connective tissue disease, human immunodeficiency virus infection, portal hypertension, congenital heart disease, or schistosomiasis)-associated types. PAH could not be interpreted solely by pathophysiological theories. The impact of the transforming growth factor-β superfamily-related genes on the development of PAH in children remains to be clarified. Pertinent literature on the transforming growth factor-β superfamily-related genes in relation to PAH in children published after the year 2000 was reviewed and analyzed. Bone morphogenetic protein receptor type II gene mutation promotes cell division or prevents cell death, resulting in an overgrowth of cells in small arteries throughout the lungs. About 20% of individuals with a bone morphogenetic protein receptor type II gene mutation develop symptomatic PAH. In heritable PAH, bone morphogenetic protein receptor type II mutations may be absent; while mutations of other genes, such as type I receptor activin receptor-like kinase 1 and the type III receptor endoglin (both associated with hereditary hemorrhagic telangiectasia), caveolin-1 and KCNK3, the gene encoding potassium channel subfamily K, member 3, can be detected, instead. Gene mutations, environmental changes and acquired adjustment, etc. may explain the development of PAH. The researches on PAH rat model and familial PAH members may facilitate the elucidations of the mechanisms and further provide theories for prophylaxis and treatment of PAH.

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Novel Mutations in BMPR2, ACVRL1 and KCNA5 Genes and Hemodynamic Parameters in Patients with Pulmonary Arterial Hypertension

Cited by 45 publications

References 42 publications

Molecular and functional characterization of the BMPR2 gene in Pulmonary Arterial Hypertension

Molecular and functional characterization of the BMPR2 gene in Pulmonary Arterial Hypertension

Novel ACLV1 Mutation Identified in Late Onset Hereditary Hemorrhagic Telangiectasia

Pulmonary artery hypertension in childhood: The transforming growth factor-β superfamily-related genes

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