Low-input and single-cell methods for Infinium DNA methylation BeadChips

Author:

Lee Sol Moe1ORCID,Loo Christian E2,Prasasya Rexxi D3,Bartolomei Marisa S3,Kohli Rahul M4,Zhou Wanding15ORCID

Affiliation:

1. Center for Computational and Genomic Medicine, The Children's Hospital of Philadelphia , PA 19104 , USA

2. Graduate Group in Biochemistry and Biophysics, University of Pennsylvania , Philadelphia , PA 19104 , USA

3. Department of Cell and Developmental Biology, Epigenetics Institute, University of Pennsylvania Perelman School of Medicine , Philadelphia , PA 19104 , USA

4. Department of Medicine, University of Pennsylvania , Philadelphia , PA 19104 , USA

5. Department of Pathology and Laboratory Medicine, University of Pennsylvania , Philadelphia , PA 19104 , USA

Abstract

Abstract The Infinium BeadChip is the most widely used DNA methylome assay technology for population-scale epigenome profiling. However, the standard workflow requires over 200 ng of input DNA, hindering its application to small cell-number samples, such as primordial germ cells. We developed experimental and analysis workflows to extend this technology to suboptimal input DNA conditions, including ultra-low input down to single cells. DNA preamplification significantly enhanced detection rates to over 50% in five-cell samples and ∼25% in single cells. Enzymatic conversion also substantially improved data quality. Computationally, we developed a method to model the background signal's influence on the DNA methylation level readings. The modified detection P-value calculation achieved higher sensitivities for low-input datasets and was validated in over 100 000 public diverse methylome profiles. We employed the optimized workflow to query the demethylation dynamics in mouse primordial germ cells available at low cell numbers. Our data revealed nuanced chromatin states, sex disparities, and the role of DNA methylation in transposable element regulation during germ cell development. Collectively, we present comprehensive experimental and computational solutions to extend this widely used methylation assay technology to applications with limited DNA.

Funder

National Institute of Health

Children's Hospital of Philadelphia

FOXO Bioscience

Publisher

Oxford University Press (OUP)

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