2000
DOI: 10.1093/hmg/9.8.1201
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Co-localisation of CCG repeats and chromosome deletion breakpoints in Jacobsen syndrome: evidence for a common mechanism of chromosome breakage

Abstract: Folate-sensitive fragile sites are associated with the expansion and hypermethylation of CCG-repeats. The fragile site in 11q23.3, FRA11B, has been shown to cause chromosome deletions in vivo, its expression being associated with Jacobsen (11q-) syndrome. However, the majority of Jacobsen deletions are distal to FRA11B and are not related to its expression. To test the hypothesis that other unidentified fragile sites might be located in 11q23.3-24 and may cause these deletions, we have identified and character… Show more

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Cited by 75 publications
(69 citation statements)
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“…We have also recently mapped the breakpoint of a patient with Jacobsen syndrome to the same repeat. 39 A further CCG repeat (TNR/11q#6) was located within PAC dJ36-N10 less than 1 Mb from the repeat TNR/11q#7.…”
Section: Localization Of Cll Deletion Breakpoints To Ccg Repeatsmentioning
confidence: 96%
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“…We have also recently mapped the breakpoint of a patient with Jacobsen syndrome to the same repeat. 39 A further CCG repeat (TNR/11q#6) was located within PAC dJ36-N10 less than 1 Mb from the repeat TNR/11q#7.…”
Section: Localization Of Cll Deletion Breakpoints To Ccg Repeatsmentioning
confidence: 96%
“…39 Nine overlapping YACs (y986C07, y984E06, y891F09, y952H06, y921B11, y795F05, y975H06, y793D09, y920C04), located within the CLL minimal deleted region, were found to contain the same trinucleotide repeat. The high density of microsatellite markers in this region of the YAC contig allowed the accurate localization of this CCG-repeat to between D11S1897 and D11S2105.…”
Section: Identification Of a Ccg Repeat Within The Minimal Deleted Rementioning
confidence: 99%
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“…In fact, the expanded and hypermethylated CGG sequence is replicating so late that (under particular culture conditions) it is not duplicated at mitosis and cannot condense at metaphase. All these fragile sites (including FRAXA, FRAXE, FRAXF, FRA10A, FRA11A, FRA11B, FRA12A, and FRA16A) are located in promoters and their expression associates with silencing of the respective genes [Oberlé et al, 1991;Knight et al, 1993;Ritchie et al, 1994;Nancarrow et al, 1995;Jones et al, 2000;Sarafidou et al, 2004;Debacker et al, 2007;Winnepenninckx et al, 2007]. …”
mentioning
confidence: 99%