The Precise Breakpoint Mapping in Paracentric Inversion 10q22.2q23.3 by Comprehensive Cytogenomic Analysis, Multicolor Banding, and Single-Copy Chromosome Sequencing

Татьяна Витальевна Карамышева, Гайнер Татьяна, Евгений Анатольевич Елисафенко, Владимир Александрович Трифонов, Эльвира Гамиловна Закирова, Константин Евгеньевич Орищенко, Прохорович А. Мария, Мария Е. Лопаткина, Николай А. Скрябин, Игорь Н. Лебедев, Николай Борисович Рубцов

Результат исследования: Научные публикации в периодических изданияхстатьярецензирование

Аннотация

Detection and precise genomic mapping of balanced chromosomal abnormalities in patients with impaired fertility or a clinical phenotype represent a challenge for current cytogenomics owing to difficulties with precise breakpoint localization in the regions enriched for DNA repeats and high genomic variation in such regions. Here, we present a comprehensive cytogenomic approach to breakpoint mapping in a rare paracentric inversion on 10q (in a patient with oligoasthenoteratozoospermia and necrozoospermia) that does not affect other phenotype traits. Multicolor banding, chromosomal microarray analysis, chromosome microdissection with reverse painting, and single-copy sequencing of the rearranged chromosome were performed to determine the length and position of the inverted region as well as to rule out a genetic imbalance at the breakpoints. As a result, a paracentric 19.251 Mbp inversion at 10q22.2q23.3 was described. The most probable location of the breakpoints was predicted using the hg38 assembly. The problems of genetic counseling associated with enrichment for repeats and high DNA variability of usual breakpoint regions were discussed. Possible approaches for cytogenomic assessment of couples with balanced chromosome rearrangements and problems like reproductive failures were considered and suggested as useful part of effective genetic counseling.
Язык оригиналаанглийский
Номер статьи3255
ЖурналBiomedicines
Том10
Номер выпуска12
DOI
СостояниеОпубликовано - 14 дек. 2022

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