Dominant-Negative
            <i>ALK2</i>
            Allele Associates With Congenital Heart Defects

Smith, K. A.; Joziasse, Irene C.; Chocron, Sonja; Dinther, Maarten van; Guryev, Victor; Verhoeven, Manon C.; Rehmann, Holger; Smagt, Jasper J. van der; Doevendans, Pieter A.; Cuppen, Edwin; Mulder, Barbara J.M.; Dijke, Peter ten; Bakkers, Jeroen

doi:10.1161/circulationaha.108.843714

Cited by 96 publications

(69 citation statements)

References 34 publications

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“…Next, endogenous ALK2 expression was knocked down by an RNAi construct as previously described. 14 Transfection with the ALK2 p.His286Asp variant demonstrated significantly lower levels of luciferase activity in the uninduced state (Po0.05), but a difference from wt ALK2 was not observed upon stimulation with BMP6 (Figure 2b). These results indicate that the ALK2 p.His286Asp receptor is capable of propagating a signal when stimulated with a BMP ligand, but this activity is impaired when the ALK2 p.His286Asp variant is in the presence of the wt ALK2 form of the receptor.…”

Section: Resultsmentioning

confidence: 96%

“…14 In the current study, we report on a patient with DS and a primum-type atrial septal defect who harbors three cSNPs in genes associated with endocardial cushion development. The cSNPs result in missense substitutions in the type I BMP receptor genes, ALK2 and ALK3, resulting in the genetic variants p.His286Asp and p.Glu414Lys, respectively, and in the epidermal growth factor receptor family gene, ERRB3, resulting in the p.Thr1169Ile variant.…”

Section: Discussionmentioning

confidence: 95%

“…One of these variants identified has a dominant-interfering effect on BMP signaling and is associated with primum-type atrial septal defect (ASD) type I. 14 Here we report an additional ALK2 variant that was identified in a patient with trisomy 21 and a primum-type ASD (ASD type I). In addition to the ALK2 variant, two other variations were detected in another type I BMP receptor gene, ALK3, and in the epidermal growth factor receptor family, ErbB3.…”

Section: Introductionmentioning

confidence: 92%

“…19 This included an injection with vector only or in combination with a short hairpin RNA, the latter to knockdown endogenous bovine ALK2 but not vector-based human ALK2, as described previously. 14 …”

Section: Constructs Luciferase Assay and Kinase Activity Assaysmentioning

confidence: 99%

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ALK2 mutation in a patient with Down's syndrome and a congenital heart defect

et al. 2011

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Down's syndrome (DS), resulting from an additional copy of chromosome 21 (trisomy 21), is frequently associated with congenital heart defects (CHDs). Although the increased dosage of chromosome 21 sequences is likely to be part of the etiology of cardiac defects, only a proportion of DS patients exhibit a congenital heart defect (birth prevalence 40-60%). Through a large-candidate gene-sequencing screen in patients with atrioventricular septal defects, substitutions were identified in bone morphogenetic protein (BMP ) type I receptor ALK2 and two other genes in a patient with DS and a primum-type atrial septal defect. Structural modeling of the cytoplasmic domain of the ALK2 receptor suggests that H286 is in close proximity to the nucleotide-binding site of the kinase domain. We investigated whether this p.His286Asp substitution altered ALK2 function by using both in vitro as well as in vivo assays. The p.His286Asp variant demonstrated impaired functional activity as measured by BMP-specific transcriptional response assays. Furthermore, mild dominant-interfering activity was observed in vivo compared with wild-type ALK2 as determined by RNA injection into zebrafish embryos. These data indicate that in the context of a DS background, ALK2-mediated reduction of BMP signaling may contribute to CHDs.

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Section: Resultsmentioning

confidence: 96%

Section: Discussionmentioning

confidence: 95%

Section: Introductionmentioning

confidence: 92%

Section: Constructs Luciferase Assay and Kinase Activity Assaysmentioning

confidence: 99%

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ALK2 mutation in a patient with Down's syndrome and a congenital heart defect

et al. 2011

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“…In this way, mutations of the ALK2 receptor identified in patients with AV septal defects were tested by injecting zebrafish with mRNA engineered to contain the putative disease-causing mutation. This induced AV canal defects, proving the causative nature of the mutation [90]. Other recent examples of reverse genetics where a putative human disease modulating gene has been validated using zebrafish include:…”

Section: The Genetics Of Cardiovascular Disease 193mentioning

confidence: 99%

The genetics of cardiovascular disease: new insights from emerging approaches

Chico¹,

Milo²,

Crossman³

2009

The Journal of Pathology

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The prospect that sequencing the human genome would see rapid translation of a greater understanding of cardiovascular genetics into novel diagnostics and therapeutics has so far met with only limited success. However, diverse technological advances and exploitation of novel animal models of cardiovascular development and disease are providing ever more insight into cardiovascular diseases and development, and bring closer the prospect of 'postgenomic' diagnostics and therapies. Here we review some of these emerging approaches (genome wide association studies, deep sequencing, microRNA regulation, and zebrafish as a model of cardiovascular disease and development) and discuss their potential for finally fulfilling the promise of application to clinical cardiovascular medicine.

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The value of the clinical geneticist caring for adults with congenital heart disease: Diagnostic yield and patients' perspective

Engelen¹,

Baars

Felix

et al. 2013

American J of Med Genetics Pt A

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For adult patients with congenital heart disease (CHD), knowledge about the origin and inheritance of their CHD is important. Clinical geneticists may play a significant role in their care. We explored the diagnostic yield of clinical genetic consultation of adult CHD patients, patients' motivations for the consultation, implications for reproductive decisions, patients' evaluation of the impact of provided information, and satisfaction with counseling. Chart review was performed on all adult patients referred for CHD to our clinical genetics department between 2000 and 2011 (n = 90). Additionally, a questionnaire was sent to those patients referred between 2005 and 2011 (n = 64), of which 46 useful questionnaires were returned (72% response). Of patients without an etiological diagnosis at referral (n = 83), 17 (20%) were eventually diagnosed with syndromic CHD, 6 (7%) with nonsyndromic monogenetic CHD and 45 (54%) with nonsyndromic multifactorial CHD. The diagnosis remained undetermined in 15 (18%) patients. Half of patients who returned the questionnaire had purposefully postponed having children until after genetic consultation and 13% had changed their mind about having children or not after the consultation. Counseling was valued positively. In this study, we showed the added value of clinical genetic consultation in the care for adult CHD patients: it improves diagnostics by establishing an etiological diagnosis and associated recurrence risk in a substantial proportion of patients and leads to more informed reproductive decisions. With new genetic testing technologies an etiological diagnosis may be established in an increasing number of patients in the near future.

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Dominant-Negative ALK2 Allele Associates With Congenital Heart Defects

Cited by 96 publications

References 34 publications

ALK2 mutation in a patient with Down's syndrome and a congenital heart defect

ALK2 mutation in a patient with Down's syndrome and a congenital heart defect

The genetics of cardiovascular disease: new insights from emerging approaches

The value of the clinical geneticist caring for adults with congenital heart disease: Diagnostic yield and patients' perspective

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