1996
DOI: 10.1002/(sici)1097-0223(199610)16:10<915::aid-pd966>3.0.co;2-v
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Microdissection and Dop-PCR-Based Reverse Chromosome Painting as a Fast and Reliable Strategy in the Analysis of Various Structural Chromosome Abnormalities

Abstract: Reverse chromosome painting has become a powerful tool in clinical genetics for the characterization of cytogenetically unclassifiable aberrations. In this report, the application of a sensitive and rapid procedure for the complete and precise identification of four different de novo structural chromosome abnormalities is presented. These chromosome rearrangements include a marker derived from chromosome 3(cen–q11), an interstitial deletion of chromosome 13 [del(13)(q14q22)], an unbalanced translocation [46,XY… Show more

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Cited by 21 publications
(7 citation statements)
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“…The majority of WHS-associated chromosome changes are de novo, and they are expected to be isolated deletions. However, unbalanced de novo translocations, consisting more often of t(4p;8p) translocations, but also including a t(4p;7p) translocation, have been reported with unexpected high frequency in WHS, and they were all maternal in origin (Wieczorek et al 2000;Zollino et al 2004;Tonnies et al 2001;Petit et al 1998;Muller-Navia et al 1996). These reports point at a great complexity of the WHS-associated chromosome defects, which can be the cause of the great phenotypic variability of this condition.…”
Section: Discussionmentioning
confidence: 99%
“…The majority of WHS-associated chromosome changes are de novo, and they are expected to be isolated deletions. However, unbalanced de novo translocations, consisting more often of t(4p;8p) translocations, but also including a t(4p;7p) translocation, have been reported with unexpected high frequency in WHS, and they were all maternal in origin (Wieczorek et al 2000;Zollino et al 2004;Tonnies et al 2001;Petit et al 1998;Muller-Navia et al 1996). These reports point at a great complexity of the WHS-associated chromosome defects, which can be the cause of the great phenotypic variability of this condition.…”
Section: Discussionmentioning
confidence: 99%
“…(ii) For reverse painting five copies of the derivative chromosome 14 (derived from peripheral blood lymphocyte metaphases of the propositus) were microdissected and amplified by DOP‐PCR as described by Guan et al [1994]. Amplified microdissected DNA was labeled with Biotin‐16‐dUTP (Roche Diagnostics) in a secondary PCR reaction according to the protocol of Müller‐Navia et al [1996]. Chromosomal in situ suppression (CISS) hybridization and detection of the biotinylated probes was carried out as described [Lichter and Cremer, 1992] with minor modifications.…”
Section: Methodsmentioning
confidence: 99%
“…Theoretically, a single cell contains ample nuclear material for PCR amplification. Whilst a number of methods for single cell PCR have been described, 13,[25][26][27][28] the small quantity of template obtained from such specimens is not readily responsive to standard methods of manipulation. Until reliable and reproducible methods for such specimens are more common-place, molecular analysis of microdissected tissue requires that many cells be acquired for each experiment.…”
Section: Downstream Applications For Microdissected Specimensmentioning
confidence: 99%