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Isothermal multiple displacement amplification: a methodical approach enhancing molecular routine diagnostics of microcarcinomas and small biopsies.

ΤίτλοςIsothermal multiple displacement amplification: a methodical approach enhancing molecular routine diagnostics of microcarcinomas and small biopsies.
Publication TypeJournal Article
Year of Publication2014
AuthorsMairinger, F. D., Walter R. Fh, Vollbrecht C., Hager T., Worm K., Ting S., Wohlschläger J., Zarogoulidis P., Zarogoulidis K., & Schmid K. W.
JournalOnco Targets Ther
Volume7
Pagination1441-7
Date Published2014
ISSN1178-6930
Abstract

BACKGROUND AND METHODS: Isothermal multiple displacement amplification (IMDA) can be a powerful tool in molecular routine diagnostics for homogeneous and sequence-independent whole-genome amplification of notably small tumor samples, eg, microcarcinomas and biopsies containing a small amount of tumor. Currently, this method is not well established in pathology laboratories. We designed a study to confirm the feasibility and convenience of this method for routine diagnostics with formalin-fixed, paraffin-embedded samples prepared by laser-capture microdissection.RESULTS: A total of 250 μg DNA (concentration 5 μg/μL) was generated by amplification over a period of 8 hours with a material input of approximately 25 cells, approximately equivalent to 175 pg of genomic DNA. In the generated DNA, a representation of all chromosomes could be shown and the presence of elected genes relevant for diagnosis in clinical samples could be proven. Mutational analysis of clinical samples could be performed without any difficulty and showed concordance with earlier diagnostic findings.CONCLUSION: We established the feasibility and convenience of IMDA for routine diagnostics. We also showed that small amounts of DNA, which were not analyzable with current molecular methods, could be sufficient for a wide field of applications in molecular routine diagnostics when they are preamplified with IMDA.

DOI10.2147/OTT.S65144
Alternate JournalOnco Targets Ther
PubMed ID25152625
PubMed Central IDPMC4140239

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