Genotyping Microarray for the Detection of More Than 200 CFTR Mutations in Ethnically Diverse Populations

Schrijver, Iris; Oitmaa, Eneli; Metspalu, Andres; Gardner, Phyllis

doi:10.1016/s1525-1578(10)60567-3

Cited by 39 publications

(29 citation statements)

References 22 publications

Supporting

Mentioning

Contrasting

Order By: Relevance

“…Highthroughput molecular genetics has changed the face of medical research dramatically, but it has perhaps had less of an impact on clinical medicine than one might expect [Tischfield et al, 2005]. For example, it is technically feasible to use gene-chip methodology to screen for any of several hundred possible mutations that cause cystic fibrosis [Schrijver et al, 2005]. However, the logistics of gene-chip development are difficult.…”

Section: Clinical and Economic Aspects Of Mutation Detectionmentioning

confidence: 99%

Assessing human germ‐cell mutagenesis in the Postgenome Era: A celebration of the legacy of William Lawson (Bill) Russell

Wyrobek

Mulvihill

Wassom

et al. 2007

Environ and Mol Mutagen

View full text Add to dashboard Cite

Birth defects, de novo genetic diseases, and chromosomal abnormality syndromes occur in ~5% of all live births, and affected children suffer from a broad range of lifelong health consequences. Despite the social and medical impact of these defects, and the 8 decades of research in animal systems that have identified numerous germ-cell mutagens, no human germ-cell mutagen has been confirmed to date. There is now a growing consensus that the inability to detect human germ-cell mutagens is due to technological limitations in the detection of random mutations rather than biological differences between animal and human susceptibility. A multidisciplinary workshop responding to this challenge convened at The Jackson Laboratory in Bar Harbor, Maine. The purpose of the workshop was to assess the applicability of an emerging repertoire of genomic technologies to studies of human germ-cell mutagenesis. Workshop participants recommended large-scale human germ-cell mutation studies be conducted using samples from donors with high-dose exposures, such as cancer survivors. Within this high-risk cohort, parents and children could be evaluated for heritable changes in (a) DNA sequence and chromosomal structure, (b) repeat sequences and minisatellites, and (c) global gene expression profiles and pathways. Participants also advocated the establishment of a bio-bank of human tissue samples from donors with well-characterized exposure, including medical and reproductive histories. This mutational resource could support large-scale, multipleendpoint studies. Additional studies could involve the examination of transgenerational effects NIH Public AccessAuthor Manuscript Environ Mol Mutagen. Author manuscript; available in PMC 2007 November 8. NIH-PA Author ManuscriptNIH-PA Author Manuscript NIH-PA Author Manuscript associated with changes in imprinting and methylation patterns, nucleotide repeats, and mitochondrial DNA mutations. The further development of animal models and the integration of these with human studies are necessary to provide molecular insights into the mechanisms of germcell mutations and to identify prevention strategies. Furthermore, scientific specialty groups should be convened to review and prioritize the evidence for germ-cell mutagenicity from common environmental, occupational, medical, and lifestyle exposures. Workshop attendees agreed on the need for a full-scale assault to address key fundamental questions in human germ-cell environmental mutagenesis. These include, but are not limited to, the following: Do human germ-cell mutagens exist? What are the risks to future generations? Are some parents at higher risk than others for acquiring and transmitting germ-cell mutations? Obtaining answers to these, and other critical questions, will require strong support from relevant funding agencies, in addition to the engagement of scientists outside the fields of genomics and germ-cell mutagenesis.

show abstract

Section: Clinical and Economic Aspects Of Mutation Detectionmentioning

confidence: 99%

Assessing human germ‐cell mutagenesis in the Postgenome Era: A celebration of the legacy of William Lawson (Bill) Russell

Wyrobek

Mulvihill

Wassom

et al. 2007

Environ and Mol Mutagen

View full text Add to dashboard Cite

show abstract

“…The APEX microarray has been developed over a decade [26] and mostly applied to diagnose genetic disease [27][28][29][30]. APEX is based on a two-step reaction; the hybridization between probe and target, and a single base extension by DNA polymerase at the polymorphic site with four unique dye-labeled dideoxy nucleotides [23,[27][28][29][30].…”

Section: Apex Detection In Blind Dna Samplesmentioning

confidence: 99%

“…APEX is based on a two-step reaction; the hybridization between probe and target, and a single base extension by DNA polymerase at the polymorphic site with four unique dye-labeled dideoxy nucleotides [23,[27][28][29][30]. The APEX assay is robust, cost-effective, and easily modified, which provides a higher power of identification of mutations (missense, deletion, insertion) or polymorphisms in heterozygous and homozygous patients when compared with other common microarray technologies [23].…”

Section: Apex Detection In Blind Dna Samplesmentioning

confidence: 99%

Two-dye based arrayed primer extension for simultaneous multigene detection in lipid metabolism

Jeenduang

Porntadavity

Nickisch‐Rosenegk

et al. 2015

Clinica Chimica Acta

View full text Add to dashboard Cite

“…34 For each mutation under interrogation, two forward and two reverse strand oligonucleotides were spotted, for a total of four data points per possible sequence variant. To reduce the background fluorescence and to avoid rehybridization of unbound oligonucleotides to the APEX slide, the slides were washed with 95°C distilled water and 100 mmol/L NaOH before the APEX reactions.…”

Section: Oligonucleotide Microchipsmentioning

confidence: 99%

Comprehensive Arrayed Primer Extension Array for the Detection of 59 Sequence Variants in 15 Conditions Prevalent Among the (Ashkenazi) Jewish Population

Schrijver

Külm

Gardner

et al. 2007

The Journal of Molecular Diagnostics

Self Cite

View full text Add to dashboard Cite

In the Ashkenazi Jewish population, serious and lethal genetic conditions occur with relatively high frequency. A single test that encompasses the majority of population-specific mutations is not currently available. For comprehensive carrier screening and molecular diagnostic purposes, we developed a population-specific and inclusive microarray. The arrayed primer extension genotyping microarray carries 59 sequence variant detection sites, of which 53 are detectable bi-directionally. These sites represent the most common variants in Tay-Sachs disease, Bloom syndrome, Canavan disease, Niemann-Pick A, familial dysautonomia, torsion dystonia, mucolipidosis type IV, Fanconi anemia, Gaucher disease, factor XI deficiency, glycogen storage disease type 1a, maple syrup urine disease, nonsyndromic sensorineural hearing loss, familial Mediterranean fever, and glycogen storage disease type III. Several mutations in the selected disorders that are not prevalent per se in the Ashkenazi Jewish populations, as well pseudodeficiency alleles, are also included in the array. The initial technical evaluation of this microarray demonstrates that it is comprehensive, robust, sensitive, specific , and easily modifiable. This cost-effective array is based on a diversely applied platform technology and is suitable for both carrier screening and disease detection in

show abstract

Genotyping Microarray for the Detection of More Than 200 CFTR Mutations in Ethnically Diverse Populations

Cited by 39 publications

References 22 publications

Assessing human germ‐cell mutagenesis in the Postgenome Era: A celebration of the legacy of William Lawson (Bill) Russell

Assessing human germ‐cell mutagenesis in the Postgenome Era: A celebration of the legacy of William Lawson (Bill) Russell

Two-dye based arrayed primer extension for simultaneous multigene detection in lipid metabolism

Comprehensive Arrayed Primer Extension Array for the Detection of 59 Sequence Variants in 15 Conditions Prevalent Among the (Ashkenazi) Jewish Population

Contact Info

Product

Resources

About