Challenges of Bringing Next Generation Sequencing Technologies to Clinical Molecular Diagnostic Laboratories

Wong, Lee‐Jun C.

doi:10.1007/s13311-012-0170-5

Cited by 25 publications

(20 citation statements)

References 75 publications

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“…The validation process should include an evaluation of the platform that is used and the downstream data analysis [108]. Platform validation establishes the performance of the sequencing platform and the different variants that can be detected by the assay [109]. Downstream data analysis validation establishes the software parameters required to accurately read sequence data and to detect the variants [109].…”

Section: Validation Of Mps Methods For Diagnostic Usementioning

confidence: 99%

“…Platform validation establishes the performance of the sequencing platform and the different variants that can be detected by the assay [109]. Downstream data analysis validation establishes the software parameters required to accurately read sequence data and to detect the variants [109]. These validation steps should establish the sensitivity, specificity and limitations of a particular assay.…”

Section: Validation Of Mps Methods For Diagnostic Usementioning

confidence: 99%

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Application of Massively Parallel Sequencing in the Clinical Diagnostic Testing of Inherited Cardiac Conditions

2014

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Sudden cardiac death in people between the ages of 1-40 years is a devastating event and is frequently caused by several heritable cardiac disorders. These disorders include cardiac ion channelopathies, such as long QT syndrome, catecholaminergic polymorphic ventricular tachycardia and Brugada syndrome and cardiomyopathies, such as hypertrophic cardiomyopathy and arrhythmogenic right ventricular cardiomyopathy. Through careful molecular genetic evaluation of DNA from sudden death victims, the causative gene mutation can be uncovered, and the rest of the family can be screened and preventative measures implemented in at-risk individuals. The current screening approach in most diagnostic laboratories uses Sanger-based sequencing; however, this method is time consuming and labour intensive. The development of massively parallel sequencing has made it possible to produce millions of sequence reads simultaneously and is potentially an ideal approach to screen for mutations in genes that are associated with sudden cardiac death. This approach offers mutation screening at reduced cost and turnaround time. Here, we will review the current commercially available enrichment kits, massively parallel sequencing (MPS) platforms, downstream data analysis and its application to sudden cardiac death in a diagnostic environment.

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Section: Validation Of Mps Methods For Diagnostic Usementioning

confidence: 99%

Section: Validation Of Mps Methods For Diagnostic Usementioning

confidence: 99%

Application of Massively Parallel Sequencing in the Clinical Diagnostic Testing of Inherited Cardiac Conditions

2014

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“…Whole genome and exome sequencing approaches are being successfully implemented in research projects [33,34], but are not yet routine strategies in diagnosis due to high costs, long turnover times (run and analysis time) and ethical issues. On the other hand, targeted resequencing using gene panel is appearing in a clinical setting due to lower sequencing costs, shorter sequencing time, simpler data analysis and greater sensitivity per gene due to the greater coverage achieved [35]. These new approaches may be ideal for diagnosis of several disorders with broad heterogenic phenotypes and genotypes [31,32], such as the mitochondrial disorders and CoQ deficiency syndromes.…”

Section: Genetic Testing Of Coq Deficiencies By Ngsmentioning

confidence: 99%

“…In consequence, a fraction of the coding regions could remain unsequenced. False-negative and false-positive rates are higher than in targeted panels, adding a layer of complexity and uncertainty to the diagnosis [35]. Post NGS, powerful bioinformatic tools are used to assess all the highthroughput data.…”

Section: Genetic Testing Of Coq Deficiencies By Ngsmentioning

confidence: 99%

Molecular diagnosis of coenzyme Q₁₀deficiency

Yubero

Montero

Armstrong

et al. 2015

Expert Review of Molecular Diagnostics

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Coenzyme Q10 (CoQ) deficiency syndromes comprise a growing number of neurological and extraneurological disorders. Primary-genetic but also secondary CoQ deficiencies have been reported. The biochemical determination of CoQ is a good tool for the rapid identification of CoQ deficiencies but does not allow the selection of candidate genes for molecular diagnosis. Moreover, the metabolic pathway for CoQ synthesis is an intricate and not well-understood process, where a large number of genes are implicated. Thus, only next-generation sequencing techniques (either genetic panels of whole-exome and -genome sequencing) are at present appropriate for a rapid and realistic molecular diagnosis of these syndromes. The potential treatability of CoQ deficiency strongly supports the necessity of a rapid molecular characterization of patients, since primary CoQ deficiencies may respond well to CoQ treatment.

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“…Although NGS has been extensively applied to effectively detect mtDNA mutations, there are still several big challenges existing in data analysis of mtDNA sequencing (8). Among them, most critical consideration is to decrease the number of false-positive and false-negative mutations, which are greatly affected by mtDNA sequencing depth, especially for those with low heteroplasmy level (9).…”

Section: Introductionmentioning

confidence: 99%

An Innovative Data Analysis Strategy For Accurate NGS Detection of Tumor mtDNA Mutations

Guo¹,

Zhou²,

Yuan³

et al. 2020

Preprint

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Background: Next generation sequencing (NGS) technology has been commonly applied to detect mtDNA mutations, which are reported to be strongly associated with cancers. However, several key challenges still exist in the bioinformatic analysis of mtDNA sequencing data, which greatly affect the detection accuracy of mtDNA mutations. Methods: Here, we systematically evaluated several key analysis procedures, including trimming, mapping and filtering, in mtDNA mutation detection of FFPE tissues, fresh tissues and plasma samples from cancer patients. Furthermore, the innovative bioinformatics pipeline integrating a newly-developed filtering algorithm was established.Results: We found that trimming procedure was essential for improving mtDNA mapping performance in plasma but not tissue samples. Mapping with rCRS-hg19 reference was strongly suggested for mtDNA mutation detection in plasma samples due to the extreme abundance of NUMTs. In addition, our results showed that the setting of 3 mismatches was most appropriate for mtDNA mutation calling. More importantly, we revealed the presence of a negative logarithmic relationship between mtDNA site sequencing depth and minimum detectable mutation frequency and thus build up an innovative and efficient filtering strategy to increase the accuracy and sensitivity of mutation detection. Finally, we verified that higher sequencing depth was required for PCR-based than capture-based enrichment strategy.Conclusions: Collectively, we established an innovative data analysis strategy, which is of great significance for improving the accuracy of mtDNA mutation detection for different types of tumor samples.

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Challenges of Bringing Next Generation Sequencing Technologies to Clinical Molecular Diagnostic Laboratories

Cited by 25 publications

References 75 publications

Application of Massively Parallel Sequencing in the Clinical Diagnostic Testing of Inherited Cardiac Conditions

Application of Massively Parallel Sequencing in the Clinical Diagnostic Testing of Inherited Cardiac Conditions

Molecular diagnosis of coenzyme Q₁₀deficiency

An Innovative Data Analysis Strategy For Accurate NGS Detection of Tumor mtDNA Mutations

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Challenges of Bringing Next Generation Sequencing Technologies to Clinical Molecular Diagnostic Laboratories

Cited by 25 publications

References 75 publications

Application of Massively Parallel Sequencing in the Clinical Diagnostic Testing of Inherited Cardiac Conditions

Application of Massively Parallel Sequencing in the Clinical Diagnostic Testing of Inherited Cardiac Conditions

Molecular diagnosis of coenzyme Q10deficiency

An Innovative Data Analysis Strategy For Accurate NGS Detection of Tumor mtDNA Mutations

Contact Info

Product

Resources

About

Molecular diagnosis of coenzyme Q₁₀deficiency