Microarray application in prenatal diagnosis: a position statement from the cytogenetics working group of the Italian Society of Human Genetics (SIGU), November 2011

被引:50
|
作者
Novelli, A. [1 ]
Grati, F. R. [2 ]
Ballarati, L. [3 ]
Bernardini, L. [1 ]
Bizzoco, D. [4 ]
Camurri, L. [5 ]
Casalone, R. [6 ,7 ]
Cardarelli, L. [8 ]
Cavalli, P. [9 ]
Ciccone, R. [10 ]
Clementi, M. [11 ]
Dalpra, L. [12 ]
Gentile, M. [13 ]
Gelli, G. [14 ]
Grammatico, P. [15 ]
Malacarne, M. [16 ]
Nardone, A. M. [17 ]
Pecile, V. [18 ]
Simoni, G. [2 ]
Zuffardi, O. [10 ]
Giardino, D. [3 ]
机构
[1] Casa Sollievo Sofferenza Hosp, IRCCS, Mendel Lab, San Giovanni Rotondo, Italy
[2] TOMA Adv Biomed Assays SpA, Busto Arsizio, VA, Italy
[3] IRCCS Ist Auxo Italiano, Lab Med Cytogenet & Mol Genet, Milan, Italy
[4] Artemisia Fetal Maternal Med Ctr, Rome, Italy
[5] RDI Rete Diagnost Italiana, Dept Genet, Padua, Italy
[6] Azienda Osp Univ Osped Circolo, SS Dipartimentale Genet, Varese, Italy
[7] Fdn Macchi, Varese, Italy
[8] Consorzio GENiMED, Lab Citotest, Padua, Italy
[9] AO Ist Ospitalieri, Serv Genet, Cremona, Italy
[10] Univ Pavia, I-27100 Pavia, Italy
[11] Univ Padua, Dipartimento Pediat, UO Complessa Genet Clin, I-35128 Padua, Italy
[12] Univ Milano Bicocca, Dipartimento Neurosci & Biotecnol Med, Monza, Italy
[13] Osped Venere, Dipartimento Genet Med, Asl Bari, Italy
[14] Ctr Salute Donna S Anna, UOSD Genet Med, Asl Rome, Italy
[15] Sapienza Univ, San Camillo Forlanini Hosp, Dept Mol Med, Rome, Italy
[16] Osped Galliera, Genet Lab, Genoa, Italy
[17] Fdn PTV Policlin Tor Vergata, Med Genet Lab, Rome, Italy
[18] IRCCS Burlo Garofalo, SC Lab Genet Med, Trieste, Italy
关键词
microarray; position statement; prenatal diagnosis; SIGU; ultrasound fetal abnormalities; COMPARATIVE GENOMIC HYBRIDIZATION; ARRAY-CGH; STRUCTURAL VARIATION; ABNORMALITIES; FETUSES; TRANSLOCATIONS; CONTROVERSIES; PREGNANCIES; CHALLENGES; COMPLEX;
D O I
10.1002/uog.11092
中图分类号
O42 [声学];
学科分类号
070206 ; 082403 ;
摘要
A precise guideline establishing chromosomal microarray analysis (CMA) applications and platforms in the prenatal setting does not exist. The controversial question is whether CMA technologies can or should soon replace standard karyotyping in prenatal diagnostic practice. A review of the recent literature and survey of the knowledge and experience of all members of the Italian Society of Human Genetics (SIGU) Committee were carried out in order to propose recommendations for the use of CMA in prenatal testing. The analysis of datasets reported in the medical literature showed a considerable 6.4% incidence of pathogenic copy number variations (CNVs) in the group of pregnancies with sonographically detected fetal abnormalities and normal karyotype. The reported CNVs are likely to have a relevant role in terms of nosology for the fetus and in the assessment of reproductive risk for the couple. Estimation of the frequency of copy number variations of uncertain significance (VOUS) varied depending on the different CMA platforms used, ranging from 04%, obtained using targeted arrays, to 912%, obtained using high-resolution whole genome single nucleotide polymorphism (SNP) arrays. CMA analysis can be considered a second-tier diagnostic test to be used after standard karyotyping in selected groups of pregnancies, namely those with single (apparently isolated) or multiple ultrasound fetal abnormalities, those with chromosomal rearrangements, even if apparently balanced, and those with supernumerary marker chromosomes. Copyright (c) 2012 ISUOG. Published by John Wiley & Sons, Ltd.
引用
收藏
页码:384 / 388
页数:5
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