N. Créau-Goldberg scite author profile

The duplication of a specific region of chromosome 21 could be respotisible for the main features of Down syndrome. To define and localize this region, we analyzed at the molecular level the DNA of two patients with partial duplication of chromosome 21. These patients belong to two groups of Down syndrome patients characterized by different partial trisomies 21: (i) duplication of the long arm, proximal to 21q22.2, and (ii) duplication of the end of the chromosome, distal to 21q22.2 We assessed the copy number of five chromosome 21 sequences (SOD], D21S17, D21S55, ETS2, and D21SI5) and found that D21S55 was duplicated in both cases.

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Maternal origin of a de novo balanced t(21q21q) identified by ets-2 polymorphism

Créau-Goldberg

Gégonne

Delabar

et al. 1987

Hum Genet

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Down syndrome critical region around D21S55 on proximal 21q22.3

et al. 2005

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We have analysed the DNA of 2 patients with many manifestations of Down syndrome and partial duplication of distinct regions of chromosome 21, respectively, q11.205→q22.300 and q22.300→qter (Rahmani et al.: Proceedings of the National Academy of Sciences of the United States of America 86:5958–5962, 1989). Assessment of the copy number of five chromosome 21 sequences (SODI, D21S17, D21S55, ETS2, and D21S15) has shown that D21S55 was duplicated in both cases. The size of the common duplicated region can be estimated between 400 and 3,000 Kb, after the results of pulsed‐field gel analysis and from the knowledge of regional mapping of the probes D21S17, D21S55, and ETS2. This region, located on the proximal part of 21q22.3,is postulated to contain genes the overexpression of which plays a major role in the pathogenesis of Down syndrome.

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