Rapid molecular assays to study human centromere genomics

Author:

Contreras-Galindo Rafael,Fischer Sabrina,Saha Anjan K.,Lundy John D.,Cervantes Patrick W.,Mourad Mohamad,Wang Claire,Qian Brian,Dai Manhong,Meng Fan,Chinnaiyan Arul,Omenn Gilbert S.,Kaplan Mark H.,Markovitz David M.

Abstract

The centromere is the structural unit responsible for the faithful segregation of chromosomes. Although regulation of centromeric function by epigenetic factors has been well-studied, the contributions of the underlying DNA sequences have been much less well defined, and existing methodologies for studying centromere genomics in biology are laborious. We have identified specific markers in the centromere of 23 of the 24 human chromosomes that allow for rapid PCR assays capable of capturing the genomic landscape of human centromeres at a given time. Use of this genetic strategy can also delineate which specific centromere arrays in each chromosome drive the recruitment of epigenetic modulators. We further show that, surprisingly, loss and rearrangement of DNA in centromere 21 is associated with trisomy 21. This new approach can thus be used to rapidly take a snapshot of the genetics and epigenetics of each specific human centromere in nondisjunction disorders and other biological settings.

Funder

National Cancer Institute

Concerned Parents for AIDS Research CPFA

National Institutes of Health

Programa de Desarrollo de Ciencias Básicas

Agencia Nacional de Investigación e Innovación

University of Michigan Undergraduate Research Opportunity Program

University of Michigan Cancer Biology Program Fellowship and the Medical Science Training Program

NIH Postbaccalaureate Research Education Program

NIH

Publisher

Cold Spring Harbor Laboratory

Subject

Genetics (clinical),Genetics

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