论文信息 - Prenatal diagnosis and fetal pathology of partial trisomy 20p–monosomy 4p resulting from paternal translocation

Prenatal diagnosis and fetal pathology of partial trisomy 20p–monosomy 4p resulting from paternal translocation

Amniocentesis was performed in view of a paternal balanced chromosomal rearrangement t(4;20)(p16;p12), inv(18)(p11q11). The pregnancy was complicated by severe oligohydramnios. The fetal karyotype was unbalanced: 46XX, der(4), t(4;20)(p16;p12), inv(18) (p11q11)pat., thus resulting in partial trisomy 2Op and monosomy 4p. In addition, the amniotic fluid alpha‐fetoprotein (AFP) became increasingly elevated with gestational age. The pregnancy was terminated at 25 weeks. The fetus presented with typical facial dysmorphic features, unilateral cleft lip and palate, severe renal hypoplasia, consistent with the 4p‐ (Wolf‐Hirschhorn) syndrome.

[1] D. Delbeke,et al. Alphafetoprotein (AFP), concanavalin A non-reactive AFP and specific acetylcholinesterase in amniotic fluid from pathological pregnancies. Predictive values for open spina bifida. , 1983, European journal of obstetrics, gynecology, and reproductive biology.

[2] G. Lazjuk,et al. The Wolf‐Hirschhorn syndrome , 1980 .

[3] N. Archidiacono,et al. Trisomy 20p from maternal t(3;20) translocation. , 1979, Journal of medical genetics.

[4] V. Riccardi,et al. Triplication of chromosome arm 20p due to inherited translocation and secondary nondisjunction. , 1979, American journal of medical genetics.

[5] R. Worton,et al. Partial trisomy 20 confirmed by gene dosage studies. , 1979, American journal of medical genetics.

[6] E. Zackai,et al. A (14;20) translocation, unbalanced, from a subject with severe congenital anomalies. Respository identification No. GM-981. , 1978, Cytogenetics and cell genetics.

[7] C. Williams,et al. Prenatal recognition of 4p- syndrome. , 1977, Journal of medical genetics.