Surveying the repair of ancient DNA from bones via high-throughput sequencing

Author:

Mouttham Nathalie12,Klunk Jennifer12,Kuch Melanie1,Fourney Ron3,Poinar Hendrik124

Affiliation:

1. McMaster Ancient DNA Centre, Department of Anthropology, McMaster University, Hamilton, ON, Canada

2. Department of Biology, McMaster University, Hamilton, ON, Canada

3. Science and Strategic Partnerships, Forensic Science and Identification Services, Royal Canadian Mounted Police, Ottawa, ON, Canada

4. Michael G. DeGroote Institute for Infectious Disease Research, McMaster University, Hamilton, ON, Canada

Abstract

DNA damage in the form of abasic sites, chemically altered nucleotides, and strand fragmentation is the foremost limitation in obtaining genetic information from many ancient samples. Upon cell death, DNA continues to endure various chemical attacks such as hydrolysis and oxidation, but repair pathways found in vivo no longer operate. By incubating degraded DNA with specific enzyme combinations adopted from these pathways, it is possible to reverse some of the post-mortem nucleic acid damage prior to downstream analyses such as library preparation, targeted enrichment, and high-throughput sequencing. Here, we evaluate the performance of two available repair protocols on previously characterized DNA extracts from four mammoths. Both methods use endonucleases and glycosylases along with a DNA polymerase-ligase combination. PreCR Repair Mix increases the number of molecules converted to sequencing libraries, leading to an increase in endogenous content and a decrease in cytosine-to-thymine transitions due to cytosine deamination. However, the effects of Nelson Repair Mix on repair of DNA damage remain inconclusive.

Publisher

Future Science Ltd

Subject

General Biochemistry, Genetics and Molecular Biology,Biotechnology

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