“…This finding suggests that one or more genes located within the duplicated region are sensitive to dosage alterations influencing brain development. Clinical features commonly reported among 32 clinically well-described patients with microscopically visible duplications spanning cytoband 5q35.1 are low birth weight, developmental delay, mental retardation, microcephaly, down-turned palpebral fissures, hypertelorism, micrognathia, dysplastic ears and congenital heart defects (Groen et al 1998;Lazjuk et al 1985;Levy et al 2002;Rodewald et al 1980;Schinzel 2003;Schroeder et al 1986). HPE was reported in two cases: a girl with a duplication of 5q32 fi qter [46,XX,der(10)t(5;10)(q31.3;q26)] and a boy with a microscopically visible 5q32->qter duplication and a 5p15 fi pter deletion, due to an inversion [46,XY, rec(5), dup q, inv(5)(p15q32)] (Lazjuk et al 1985;Schroeder et al 1986).…”