Deletion of the TSC2 and PKD1 genes associated with severe infantile polycystic kidney disease — a contiguous gene syndrome

Brook-Carter, P T; Peral, Belén; Ward, Christopher J.; Thompson, Peter; Hughes, Jim R.; Maheshwar, Magitha M.; Nellist, Mark; Gamble, Vicki; Harris, Peter C.; Sampson, Julian R.

doi:10.1038/ng1294-328

Cited by 445 publications

(214 citation statements)

References 22 publications

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“…Disruption of both TSC2 and PKD1 genes is associated with a severe renal phenotype presenting in infancy. 21,22 These patients have bilateral polycystic renal disease and often grossly enlarged kidneys. Hence, the PKD is more severe than that associated with mutation to just PKD1, which normally results in adult onset disease; suggesting a synergistic role for the PKD1 and TSC2 products in cyst development.…”

Section: Discussionmentioning

confidence: 99%

Identification of a subtle t(16;19)(p13.3;p13.3) in an infant with multiple congenital abnormalities using a 12-colour multiplex FISH telomere assay, M-TEL

et al. 2000

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There is increasing evidence that cytogenetically invisible chromosome rearrangements are an important cause of genetic disease. Clues to the chromosomal location of these rearrangements may be provided by a specific clinical diagnosis, which can then be investigated by targeted FISH or molecular studies. However, the phenotypic features of some microdeletion syndromes are difficult to recognise, particularly in infants. In addition, the presence of other chromosome aneuploidy may mask the typical clinical features. In the present study, the presence of tubers on cranial magnetic resonance imaging (

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Section: Discussionmentioning

confidence: 99%

Identification of a subtle t(16;19)(p13.3;p13.3) in an infant with multiple congenital abnormalities using a 12-colour multiplex FISH telomere assay, M-TEL

et al. 2000

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“…16 and 4, for ADPKD 1 and ADPKD 2 respectively to those of MFS and CCA, is worth noting and chromosomal crossovers cannot be ruled out. In tuberous sclerosis, large deletions, disrupting PKD 1 and the adjacent tuberous sclerosis type 2 gene (TSC 2) occurs, resulting in tuberous sclerosis and severe, childhood-onset polycystic kidney disease (15). So far, this has been the only clear description of a genotype/phenotype correlation in ADPKD and there are no reports of specific PKD 1 or PKD 2 mutations specifically predisposing to additional connective tissue abnormalities.…”

Section: Discussionmentioning

confidence: 99%

Polycystic kidney disease in a patient with achondroplasia

McLigeyo

Kisiangani²

2004

E Af Med Jrnl

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SUMMARYAutosomal dominant polycystic kidney disease is a multisystem disease involving many organs. An association with other diseases such as tuberous sclerosis, von Hippel-Lindau disease and Marfan syndrome have been previously described. We describe a 35 year old female with achondroplasia who developed polycystic kidney disease involving both kidneys and progressing to end-stage renal disease. To the best of our knowledge this is the first such case described in the literature. We also delve, briefly, into the possibility of the genes and chromosomes involved in Marfan syndrome, polycystic kidney disease, tuberous sclerosis and achondroplasia playing a role in the co-occurrence of these entities.

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“…A contiguous gene syndrome involving deletions of PKD1 and TSC2 has also been described where patients develop severe early-onset PKD with ESRF in childhood. 43 In the PKD1 gene, the location of the mutation appears to influence the disease severity with mutations in the 5 0 portion of the gene (0 -7812 nt) associated with a lower Polycystic kidney disease C Boucher and R Sandford mean age of ESRF than those 3 0 of 7812 nt. 44 In addition, it has been shown that a population of PKD1 patients presenting with a vascular phenotype have a median position of mutation located more 5 0 than a control population.…”

Section: Mutationsmentioning

confidence: 99%

Autosomal dominant polycystic kidney disease (ADPKD, MIM 173900, PKD1 and PKD2 genes, protein products known as polycystin-1 and polycystin-2)

Boucher

Sandford

2004

Eur J Hum Genet

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Autosomal dominant polycystic kidney disease (ADPKD) is a common inherited nephropathy affecting over 1:1000 of the worldwide population. It is a systemic condition with frequent hepatic and cardiovascular manifestations in addition to the progressive development of renal cysts that eventually result in loss of renal function in the majority of affected individuals. The diagnosis of ADPKD is typically made using renal imaging despite the identification of mutations in PKD1 and PKD2 that account for virtually all cases. Mutations in PKD1 are associated with more severe clinical disease and earlier onset of renal failure. Most PKD gene mutations are loss of function and a 'two-hit' mechanism has been demonstrated underlying focal cyst formation. The protein products of the PKD genes, the polycystins, form a calcium-permeable ion channel complex that regulates the cell cycle and the function of the renal primary cilium. Abnormal cilial function is now thought to be the primary defect in several types of PKD including autosomal recessive polycystic kidney disease and represents a novel and exciting mechanism underlying a range of human diseases.

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Deletion of the TSC2 and PKD1 genes associated with severe infantile polycystic kidney disease — a contiguous gene syndrome

Cited by 445 publications

References 22 publications

Identification of a subtle t(16;19)(p13.3;p13.3) in an infant with multiple congenital abnormalities using a 12-colour multiplex FISH telomere assay, M-TEL

Identification of a subtle t(16;19)(p13.3;p13.3) in an infant with multiple congenital abnormalities using a 12-colour multiplex FISH telomere assay, M-TEL

Polycystic kidney disease in a patient with achondroplasia

Autosomal dominant polycystic kidney disease (ADPKD, MIM 173900, PKD1 and PKD2 genes, protein products known as polycystin-1 and polycystin-2)

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