W. R. Wells scite author profile

BackgroundArray Comparative Genomic Hybridization (a-CGH) is a powerful molecular cytogenetic tool to detect genomic imbalances and study disease mechanism and pathogenesis. We report our experience with the clinical implementation of this high resolution human genome analysis, referred to as Chromosomal Microarray Analysis (CMA).Methods and FindingsCMA was performed clinically on 2513 postnatal samples from patients referred with a variety of clinical phenotypes. The initial 775 samples were studied using CMA array version 4 and the remaining 1738 samples were analyzed with CMA version 5 containing expanded genomic coverage. Overall, CMA identified clinically relevant genomic imbalances in 8.5% of patients: 7.6% using V4 and 8.9% using V5. Among 117 cases referred for additional investigation of a known cytogenetically detectable rearrangement, CMA identified the majority (92.5%) of the genomic imbalances. Importantly, abnormal CMA findings were observed in 5.2% of patients (98/1872) with normal karyotypes/FISH results, and V5, with expanded genomic coverage, enabled a higher detection rate in this category than V4. For cases without cytogenetic results available, 8.0% (42/524) abnormal CMA results were detected; again, V5 demonstrated an increased ability to detect abnormality. Improved diagnostic potential of CMA is illustrated by 90 cases identified with 51 cryptic microdeletions and 39 predicted apparent reciprocal microduplications in 13 specific chromosomal regions associated with 11 known genomic disorders. In addition, CMA identified copy number variations (CNVs) of uncertain significance in 262 probands; however, parental studies usually facilitated clinical interpretation. Of these, 217 were interpreted as familial variants and 11 were determined to be de novo; the remaining 34 await parental studies to resolve the clinical significance.ConclusionsThis large set of clinical results demonstrates the significantly improved sensitivity of CMA for the detection of clinically relevant genomic imbalances and highlights the need for comprehensive genetic counseling to facilitate accurate clinical correlation and interpretation.

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Direct Adaptive and Neural Control of Wing-Rock Motion of Slender Delta Wings

Singh

Yirn

Wells

1995

Journal of Guidance, Control, and Dynamics

138

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Chemical surface preparation for metallization of stereolithography polymers

Luan

Yeung

Wells

et al. 2000

Applied Surface Science

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Heat Transfer Aspects of Nonisothermal Axisymmetric Upset Forging

Dadras

Wells

1984

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A finite difference solution for the transient heat transfer during axisymmetric upset forging has been developed. The interfacial film between the die and the billet has been included in the analysis, and all modes of heat transfer have been taken into account. The results of a parallel experimental study have also been presented. The effects of geometrical and physical characteristics of the billet and the die on the heat transfer process, particularly on die heating, have been systematically investigated.

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Optimal evasive tactics against a proportional navigation missile with time delay.

Slater

Wells

1973

Journal of Spacecraft and Rockets

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W. R. Wells

Clinical Implementation of Chromosomal Microarray Analysis: Summary of 2513 Postnatal Cases

Direct Adaptive and Neural Control of Wing-Rock Motion of Slender Delta Wings

Chemical surface preparation for metallization of stereolithography polymers

Heat Transfer Aspects of Nonisothermal Axisymmetric Upset Forging

Optimal evasive tactics against a proportional navigation missile with time delay.

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