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BMC Medical Genetics (1)
Diabetes Care (1)
Journal of Medical Genetics (1)
Authors
Abramowicz, Marc J (2)
Abramowicz, Daniel (1)
Abramowicz, Marc J. (1)
Christophe, Daniel (1)
Christophe-Hobertus, Christiane (1)
David, Karen L (1)
Deconinck, Hilde (1)
Desir, Julie (1)
Gecz, Jozef (1)
Ghisdal, Lidia (1)
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Year of Publication
2011 (1)
2007 (1)
2004 (1)
Document Types
research-article (2)
case-report (1)
1.  New-Onset Diabetes After Renal Transplantation 
Ghisdal, Lidia | Van Laecke, Steven | Abramowicz, Marc J. | Vanholder, Raymond | Abramowicz, Daniel
Diabetes Care  2011;35(1):181-188.
doi:10.2337/dc11-1230
PMCID: PMC3241330  PMID: 22187441
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2.  Borate transporter SLC4A11 mutations cause both Harboyan syndrome and non‐syndromic corneal endothelial dystrophy 
Desir, Julie | Moya, Graciela | Reish, Orit | Van Regemorter, Nicole | Deconinck, Hilde | David, Karen L | Meire, Françoise M | Abramowicz, Marc J
Journal of Medical Genetics  2007;44(5):322-326.
Harboyan syndrome, or corneal dystrophy and perceptive deafness (CDPD), consists of congenital corneal endothelial dystrophy and progressive perceptive deafness, and is transmitted as an autosomal recessive trait. CDPD and autosomal recessive, non‐syndromic congenital hereditary endothelial corneal dystrophy (CHED2) both map at overlapping loci at 20p13, and mutations of SLC4A11 were reported recently in CHED2. A genotype study on six families with CDPD and on one family with either CHED or CDPD, from various ethnic backgrounds (in the seventh family, hearing loss could not be assessed because of the proband's young age), is reported here. Novel SLC4A11 mutations were found in all patients. Why some mutations cause hearing loss in addition to corneal dystrophy is presently unclear. These findings extend the implication of the SLC4A11 borate transporter beyond corneal dystrophy to perceptive deafness.
doi:10.1136/jmg.2006.046904
PMCID: PMC2597979  PMID: 17220209
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3.  TM4SF10 gene sequencing in XLMR patients identifies common polymorphisms but no disease-associated mutation 
Christophe-Hobertus, Christiane | Kooy, Frank | Gecz, Jozef | Abramowicz, Marc J | Holinski-Feder, Elke | Schwartz, Charles | Christophe, Daniel
BMC Medical Genetics  2004;5:22.
Background
The TM4SF10 gene encodes a putative four-transmembrane domains protein of unknown function termed Brain Cell Membrane Protein 1 (BCMP1), and is abundantly expressed in the brain. This gene is located on the short arm of human chromosome X at p21.1. The hypothesis that mutations in the TM4SF10 gene are associated with impaired brain function was investigated by sequencing the gene in individuals with hereditary X-linked mental retardation (XLMR).
Methods
The coding region (543 bp) of TM4SF10, including intronic junctions, and the long 3' untranslated region (3 233 bp), that has been conserved during evolution, were sequenced in 16 male XLMR patients from 14 unrelated families with definite, or suggestive, linkage to the TM4SF10 gene locus, and in 5 normal males.
Results
Five sequence changes were identified but none was found to be associated with the disease. Two of these changes correspond to previously known SNPs, while three other were novel SNPs in the TM4SF10 gene.
Conclusion
We have investigated the majority of the known MRX families linked to the TM4SF10 gene region. In the absence of mutations detected, our study indicates that alterations of TM4SF10 are not a frequent cause of XLMR.
doi:10.1186/1471-2350-5-22
PMCID: PMC517934  PMID: 15345028
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