论文信息 - Prenatal diagnosis of Niemann-Pick type C disease: current strategy from an experience of 37 pregnancies at risk. - 字舞流文

Prenatal diagnosis of Niemann-Pick type C disease: current strategy from an experience of 37 pregnancies at risk.

Thirty-seven pregnancies at risk for Niemann-Pick type C disease were monitored by study of cultured amniotic fluid cells (8 cases) or chorionic villus cells (29 cases) in 23 couples over the period 1984-91. An early protocol combined determination of sphingomyelinase activity with electron microscopy. The current strategy, based on the demonstration of specific abnormalities in intracellular processing of exogenous cholesterol, combines the study of the early phase (first 6 h) of LDL-induced cholesteryl ester formation and the histochemical evaluation (filipin staining after 24 h of LDL uptake) of the LDL-induced accumulation of unesterified cholesterol. Thirteen fetuses were predicted to be affected. Confirmation of the diagnosis was made by study of cholesterol processing in fetal skin fibroblast cultures and/or by demonstration of a characteristic lipid storage in fetal liver, already present at 14 w gestation. Definition of the biochemical phenotype (classical, variant, or intermediate) of the index case, with regard to cholesterol-processing abnormalities, is an absolute prerequisite to adequate genetic counseling in a given family. Prenatal diagnosis has now proved a safe procedure in the predominant (approximately 85%) group of families with the classical phenotype.

R. Rousson | M. Vanier | P. Pentchev | J. Boué | C. Rodriguez-Lafrasse | C. Dumontel | A. Choiset | M. Juge | G. Mandon | M. Peyrat | Agnès Choiset | Claire Rodriguez-Lafrasse | Peter G. Pentchev | Marie T. Vanier | Marie-Christine Juge | P. Louisot | Ginette Mandon | Joëlle Boué | Christiane Dumontel | A. Revol

[1] A. Chabás,et al. [Type C Niemann-Pick disease]. , 1991, Sangre.

[2] R. Brady,et al. Type C Niemann-Pick disease: cellular uncoupling of cholesterol homeostasis is linked to the severity of disruption in the intracellular transport of exogenously derived cholesterol. , 1991, Biochimica et biophysica acta.

[3] R. Rousson,et al. Type C Niemann-Pick disease: spectrum of phenotypic variation in disruption of intracellular LDL-derived cholesterol processing. , 1991, Biochimica et biophysica acta.

[4] G. Mieli-Vergani,et al. Fetal ascites: an unusual presentation of Niemann-Pick disease type C. , 1989, Archives of disease in childhood.

[5] L. Liscum,et al. The intracellular transport of low density lipoprotein-derived cholesterol is defective in Niemann-Pick type C fibroblasts , 1989, The Journal of cell biology.

[6] R. Brady,et al. Niemann‐Pick disease group C: clinical variability and diagnosis based on defective cholesterol esterification: A collaborative study on 70 patients , 1988, Clinical genetics.

[7] R. Brady,et al. Group C Niemann‐Pick disease: faulty regulation of low‐density lipoprotein uptake and cholesterol storage in cultured fibroblasts , 1987, FASEB journal : official publication of the Federation of American Societies for Experimental Biology.

[8] S. Patel,et al. Type C Niemann-Pick disease. A parallel loss of regulatory responses in both the uptake and esterification of low density lipoprotein-derived cholesterol in cultured fibroblasts. , 1986, The Journal of biological chemistry.

[9] S. Patel,et al. Type C Niemann-Pick disease. Abnormal metabolism of low density lipoprotein in homozygous and heterozygous fibroblasts. , 1986, The Journal of biological chemistry.

[10] R. Brady,et al. A defect in cholesterol esterification in Niemann-Pick disease (type C) patients. , 1985, Proceedings of the National Academy of Sciences of the United States of America.

[11] M. Vanier,et al. Niemann‐Pick disease type B: first‐trimester prenatal diagnosis on chorionic villi and biochemical study of a foetus at 12 weeks of development , 1985, Clinical genetics.

[12] R. Rousson,et al. Biochemical studies in Niemann‐Pick disease. III: In vitro and in vivo assays of sphingomyelin degradation in cultured skin fibroblasts and amniotic fluid cells for the diagnosis of the various forms of the disease , 1985, Clinical genetics.

[13] E. Hartree,et al. Determination of protein: a modification of the Lowry method that gives a linear photometric response. , 1972, Analytical biochemistry.

[14] R. Rousson,et al. Pathophysiological Approach of Niemann-Pick Disease Type C: Definition of a Biochemical Heterogeneity and Reevaluation of the Lipid Storage Process , 1988 .

[15] H. Kruth,et al. Niemann-pick variant disorders: comparison of errors of cellular cholesterol homeostasis in group D and group C fibroblasts. , 1987, Proceedings of the National Academy of Sciences of the United States of America.

[16] R. Rousson,et al. Sphingomyelinase and Niemann-Pick Disease , 1986 .

[17] M. Brown,et al. Receptor-mediated endocytosis of low-density lipoprotein in cultured cells. , 1983, Methods in enzymology.

[18] C. Scriver,et al. Niemann-Pick disease: prenatal diagnoses and studies of sphingomyelinase activities. , 1978, American journal of medical genetics.

[19] L. Samuels,et al. I – Biochemical Studies , 1969 .

[20] K. C. Richardson,et al. Embedding in epoxy resins for ultrathin sectioning in electron microscopy. , 1960, Stain technology.