Bi-allelic Mutations in PKD1L1 Are Associated with Laterality Defects in Humans

Vetrini, Francesco; D’Alessandro, Lisa C.A.; Akdemir, Zeynep Coban; Braxton, Alicia; Azamian, Mahshid S.; Eldomery, Mohammad K.; Miller, Kathryn; Kois, Chelsea; Sack, Virginia; Shur, Natasha; Rijhsinghani, Asha; Chandarana, Jignesh; Ding, Yan; Holtzman, Judy; Jhangiani, Shalini N.; Muzny, Donna M.; Gibbs, Richard A.; Eng, Christine M.; Hanchard, Neil A.; Harel, Tamar; Rosenfeld, Jill A.; Belmont, John W.; Lupski, James R.; Yang, Yaping

doi:10.1016/j.ajhg.2016.07.011

Cited by 59 publications

(55 citation statements)

References 46 publications

(91 reference statements)

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“…Of the nine PKD1L1 variants (six missense, two splice‐site, and one chain‐terminating), eight have yet to be associated with a disease phenotype. The splice site mutation found in subject 3 (c.6473+2_6473+3delTG) was recently reported as a homozygous variant in 2 siblings with heterotaxy and severe congenital heart disease . The variants c.T2399C (p.I800T) and c.C6949T (p.R2317W) were both present in homozygous form in subject 1 and present as heterozygous alleles in subjects 2, 6, and 7 (Table ; Supporting Table ).…”

Section: Resultsmentioning

confidence: 71%

“…In particular, PKD1L1 , which encodes the polycystin 1‐like 1 protein (a member of the polycystin protein family), had potentially pathogenic biallelic and heterozygous variants in multiple BASM participants. Given the role of PKD1L1 in ciliary calcium signaling and laterality determination, its interactions with PKD2, and its identification as a cause of complex congenital heart disease in children, further investigations of PKD1L1 variants in this BASM cohort were pursued …”

Section: Resultsmentioning

confidence: 99%

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Identification of Polycystic Kidney Disease 1 Like 1 Gene Variants in Children With Biliary Atresia Splenic Malformation Syndrome

Berauer¹,

Mezina²,

Okou³

et al. 2019

Hepatology

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Biliary atresia (BA) is the most common cause of end‐stage liver disease in children and the primary indication for pediatric liver transplantation, yet underlying etiologies remain unknown. Approximately 10% of infants affected by BA exhibit various laterality defects (heterotaxy) including splenic abnormalities and complex cardiac malformations—a distinctive subgroup commonly referred to as the biliary atresia splenic malformation (BASM) syndrome. We hypothesized that genetic factors linking laterality features with the etiopathogenesis of BA in BASM patients could be identified through whole‐exome sequencing (WES) of an affected cohort. DNA specimens from 67 BASM subjects, including 58 patient–parent trios, from the National Institute of Diabetes and Digestive and Kidney Diseases–supported Childhood Liver Disease Research Network (ChiLDReN) underwent WES. Candidate gene variants derived from a prespecified set of 2,016 genes associated with ciliary dysgenesis and/or dysfunction or cholestasis were prioritized according to pathogenicity, population frequency, and mode of inheritance. Five BASM subjects harbored rare and potentially deleterious biallelic variants in polycystic kidney disease 1 like 1 (PKD1L1), a gene associated with ciliary calcium signaling and embryonic laterality determination in fish, mice, and humans. Heterozygous PKD1L1 variants were found in 3 additional subjects. Immunohistochemical analysis of liver from the one BASM subject available revealed decreased PKD1L1 expression in bile duct epithelium when compared to normal livers and livers affected by other noncholestatic diseases. Conclusion: WES identified biallelic and heterozygous PKD1L1 variants of interest in 8 BASM subjects from the ChiLDReN data set; the dual roles for PKD1L1 in laterality determination and ciliary function suggest that PKD1L1 is a biologically plausible, cholangiocyte‐expressed candidate gene for the BASM syndrome.

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Section: Resultsmentioning

confidence: 71%

Section: Resultsmentioning

confidence: 99%

Identification of Polycystic Kidney Disease 1 Like 1 Gene Variants in Children With Biliary Atresia Splenic Malformation Syndrome

Berauer¹,

Mezina²,

Okou³

et al. 2019

Hepatology

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“…This triggers asymmetric gene expression in the lateral plate mesoderm, eventually leading to asymmetric heart looping. Due to the role of cilia in determining LR patterning, mutations affecting ciliary motility 100 and sensing 101 machinery result in HTX and CHD.…”

Section: Biological Pathways In Chdmentioning

confidence: 99%

“…Some of the “unexplained CHD cases” could be due to mutations affecting the as of yet underexplored non-coding DNA, somatic mutations and gene-environment interactions as discussed below. In addition, CHD due to biallelic mutations has been underexplored, and thus far has largely focused on candidate gene analysis and familial CHD 101 . As new statistical approaches are coupled with larger CHD cohorts, the inherent challenges in an unbiased analysis of recessive mutations in sporadic CHD can be surmounted.…”

Section: Future Efforts In Chd Genomicsmentioning

confidence: 99%

Genetics and Genomics of Congenital Heart Disease

Zaidi

Brueckner

2017

Circulation Research

393

432

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Congenital heart disease is the most common birth defect, and due to major advances in medical and surgical management, there are now more adults living with CHD than children. Until recently, the cause of the majority of CHD was unknown. Advances in genomic technologies have discovered the genetic etiology of a significant fraction of CHD, while at the same time pointing to remarkable complexity in CHD genetics. This review will focus on the evidence for genetic causes underlying CHD and discuss data supporting both monogenic and complex genetic mechanisms underlying CHD. The discoveries from CHD genetic studies draw attention to biological pathways that simultaneously open the door to a better understanding of cardiac development, and impact clinical care of CHD patients. Finally, we address clinical genetic evaluation of patients and families affected by CHD.

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“…Such mutations most commonly affect genes for cardiac transcription factors, signaling molecules or cellular structures without significantly reducing reproductive potential (40, 41). For example, mutations in the NKX2.5 gene, a critical transcription factor that specifies cardiac mesoderm during embryogenesis, were some of the first mutations associated with inherited CHD.…”

Section: The Genetics Of Chdmentioning

confidence: 99%

The genetics of congenital heart disease… understanding and improving long-term outcomes in congenital heart disease: a review for the general cardiologist and primary care physician

Simmons¹,

Brueckner²

2017

Current Opinion in Pediatrics

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Purpose of the Review This review has two purposes: 1) To provide an updated review of the genetic causes of congenital heart disease (CHD) and the clinical implications of these genetic mutations; 2) To provide a clinical algorithm for clinicians considering a genetics evaluation of a CHD patient. Recent Findings A large portion of congenital heart disease is thought to have a significant genetic contribution, and at this time a genetic cause can be identified in approximately 35% of patients. Through the advances made possible by next generation sequencing, many of the comorbidities that are frequently seen in patients with genetic congenital heart disease patients can be attributed to the genetic mutation that caused the congenital heart disease. These comorbidities are both cardiac and non-cardiac and include: neurodevelopmental disability, pulmonary disease, heart failure, renal dysfunction, arrhythmia and an increased risk of malignancy. Identification of the genetic cause of congenital heart disease helps reduce patient morbidity and mortality by improving preventive and early intervention therapies to address these comorbidities. Summary Through an understanding of the clinical implications of the genetic underpinning of congenital heart disease, clinicians can provide care tailored to an individual patient and continue to improve the outcomes of congenital heart disease patients.

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Bi-allelic Mutations in PKD1L1 Are Associated with Laterality Defects in Humans

Cited by 59 publications

References 46 publications

Identification of Polycystic Kidney Disease 1 Like 1 Gene Variants in Children With Biliary Atresia Splenic Malformation Syndrome

Identification of Polycystic Kidney Disease 1 Like 1 Gene Variants in Children With Biliary Atresia Splenic Malformation Syndrome

Genetics and Genomics of Congenital Heart Disease

The genetics of congenital heart disease… understanding and improving long-term outcomes in congenital heart disease: a review for the general cardiologist and primary care physician

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