Full karyotyping, rapid aneuploidy diagnosis or both when invasive prenatal testing is performed for diagnosis of thalassaemia?

Tse KY; Leung WC; Leung KY; Lee CP; Ng LK; Lau ET; Chan V; Tang MH

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Full karyotyping, rapid aneuploidy diagnosis or both when invasive prenatal testing is performed for diagnosis of thalassaemia?

机译：在进行有创性产前检测以诊断地中海贫血时，进行全面核型分析，快速非整倍性诊断或两者兼而有之？

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A retrospective study was performed to compare the detection rate of chromosomal abnormalities by different approaches of full karyotyping, rapid aneuploidy diagnosis (RAD) or both when invasive prenatal testing is performed for diagnosis of thalassaemia. The karyotype results of 1120 prenatal samples obtained from thalassaemia couples from January 1985 to December 2002 in a referral centre for prenatal diagnosis were studied. The detection rate of chromosomal abnormalities by four different approaches were compared: (i) karyotyping for all samples; (ii) RAD (21,18,13,X,Y) for all samples; (iii) RAD for all samples + karyotyping for cases with ultrasound abnormalities; and (iv) RAD (21,18,13) for all + RAD (X,Y) for cases with ultrasound abnormalities consistent with Turner syndrome + karyotyping for cases with ultrasound abnormalities. Normal karyotypes were found in 1103 samples (98.5%). There were 17 cases (1.5%) of chromosomal abnormalities: four cases (0.36%) were clinically significant, eight cases (0.7%) were of borderline clinical significance and five cases (0.44%) were not confirmed by subsequent prenatal or postnatal tests. The incidences of autosomal (7/1120 = 0.63%) and sex chromosomal (5/1120 = 0.45%) abnormalities were not higher than those (0.41 and 0.22%, respectively) from newborn surveys (Hook and Hamerton, 1977) (P = 0.398 and 0.216, respectively). Approach 1 would detect all 17 chromosomal abnormalities. Approach 2 would detect three of four clinically significant chromosomal abnormalities but not detect six of eight chromosomal abnormalities of borderline clinical significance and three of five chromosomal abnormalities not confirmed by subsequent prenatal or postnatal tests. Approach 3, in addition, would be able to detect all four clinically significant chromosomal abnormalities. Approach 4 would detect all four clinically significant chromosomal abnormalities but would not detect seven of eight chromosomal abnormalities of borderline clinical significance and four of five chromosomal abnormalities not confirmed by subsequent prenatal or postnatal tests. RAD (21,18,13) for all + RAD (X,Y) for cases with ultrasound abnormalities consistent with Turner syndrome + karyotyping for cases with ultrasound abnormalities seemed to be the best approach for the detection of chromosomal abnormalities when invasive prenatal testing is performed for diagnosis of thalassaemia.

机译：进行了一项回顾性研究，以比较在进行有创性产前检测以诊断地中海贫血时，通过完全核型分析，快速非整倍性诊断（RAD）或两者的不同方法对染色体异常的检测率。研究了1985年1月至2002年12月在引产前诊断转诊中心从地中海贫血夫妇那里获得的1120份产前样品的核型结果。比较了四种不同方法对染色体异常的检出率：（i）所有样品的核型分析; （ii）所有样品的RAD（21,18,13，X，Y）; （iii）对所有样本均进行RAD +超声异常病例的核型分析; （iv）对于超声异常符合特纳综合征的患者，均需RAD（21,18,13）+ RAD（X，Y），对于超声异常则应采用核型分析。在1103个样本中发现了正常的核型（98.5％）。染色体异常17例（1.5％）：4例（0.36％）有临床意义，8例（0.7％）具有临界临床意义，5例（0.44％）未通过随后的产前或产后检查确认。新生儿调查（Hook和Hamerton，1977）的常染色体异常（7/1120 = 0.63％）和性染色体异常（5/1120 = 0.45％）的发生率不高于（分别为0.41和0.22％）（P =分别为0.398和0.216）。方法1将检测所有17个染色体异常。方法2将检测到四个临床上显着的染色体异常中的三个，但不能检测到具有临界临床意义的八个染色体异常中的六个，以及未通过后续的产前或产后检查确认的五个染色体异常中的三个。此外，方法3将能够检测所有四个临床上显着的染色体异常。方法4将检测所有四个临床上显着的染色体异常，但不会检测到具有临界临床意义的八个染色体异常中的七个，以及未通过后续的产前或产后检查确认的五个染色体异常中的四个。 RAD（21,18,13）所有人+ RAD（X，Y）符合特纳综合征的超声异常病例+核型分析适用于超声异常病例似乎是在进行有创产前检查时检测染色体异常的最佳方法用于诊断地中海贫血。

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《Molecular human reproduction.》 |2006年第1期|共5页
作者
Tse KY; Leung WC; Leung KY; Lee CP; Ng LK; Lau ET; Chan V; Tang MH;
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正文语种 eng
中图分类基础医学;
关键词
teratologic; prenatal; Diagnostic; Ultrasonic; Thalassemia; 贫血; 珠蛋白生成障碍性;

机译：teratologic;prenatal;Diagnostic;Ultrasonic;Thalassemia;贫血;珠蛋白生成障碍性;

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1. Full karyotyping, rapid aneuploidy diagnosis or both when invasive prenatal testing is performed for diagnosis of thalassaemia? [J] . K.Y. Tse, W.C. Leung, K.Y. Leung, Molecular Human Reproduction . 2006,第1期

机译：在进行有创性产前检查以诊断地中海贫血时，进行全面核型分析，快速非整倍性诊断或两者兼而有之？
2. Evaluation of non-invasive prenatal testing (NIPT) for aneuploidy in an NHS setting: a reliable accurate prenatal non-invasive diagnosis (RAPID) protocol [J] . Melissa Hill, David Wright, Rebecca Daley, BMC Pregnancy and Childbirth . 2014,第1期

机译：在NHS环境中评估非整倍性的非侵入性产前检测（NIPT）：可靠，准确的产前非侵入性诊断（RAPID）方案
3. Karyotyping or rapid aneuploidy detection in prenatal diagnosis? The different views of users and providers of prenatal care. [J] . Boormans EM, Birnie E, Bilardo CM BJOG: an international journal of obstetrics and gynaecology . 2009,第10期

机译：核型分析或快速非整倍性检测在产前诊断中的作用？产前保健使用者和提供者的不同看法。
4. Prenatal Diagnosis of Aneuploidy Using Artificial Neural Networks in Relation to Health Economics [C] . A.C. Neocleous, C.K. Neocleous, N. Petkov Mediterranean Conference on Medical and Biological Engineering and Computin . 2016

机译：用人工神经网络与卫生经济学相关的非倍性产前诊断
5. Utilization of FISH technology in prenatal diagnosis to detect chromosomal aneuploidy. [D] . McCue, Erin Christine. 2000

机译：FISH技术在产前诊断中用于检测染色体非整倍性。
6. Evaluation of non-invasive prenatal testing (NIPT) for aneuploidy in an NHS setting: a reliable accurate prenatal non-invasive diagnosis (RAPID) protocol [O] . Melissa Hill, David Wright, Rebecca Daley, 2014

机译：在NHS环境中评估非整倍性的非侵入性产前检测（NIPT）：可靠准确的产前非侵入性诊断（RAPID）方案
7. Full karyotyping, rapid aneuploidy diagnosis or both when invasive prenatal testing is performed for diagnosis of thalassaemia? [O] . K.Y. Tse, W.C. Leung, K.Y. Leung, 2006

机译：在侵入性产前试验进行诊断时，全核型，快速的交氮体倍性诊断或两者均用于诊断血症？

Full karyotyping, rapid aneuploidy diagnosis or both when invasive prenatal testing is performed for diagnosis of thalassaemia?

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