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논문 기본 정보

자료유형
학술저널
저자정보
Kwon Seong Gyu (Department of Anatomy School of Medicine Kyungpook National University) Bae Geon Hue (Department of Anatomy School of Medicine Kyungpook National University) 최준혁 (경북대학교) MALINANDAMAYA (경북대학교) 전미숙 (경북대학교) 김동선 (경북대학교) Han Man-Hoon (Department of Pathology School of Medicine Kyungpook National University Daegu Korea) Park Seongyeol (Graduate School of Medical Science and Engineering (GSMSE) Korea Advanced Institute of Science and) Ju Young Seok (Graduate School of Medical Science and Engineering (GSMSE) Korea Advanced Institute of Science and) Choi Seock Hwan (Department of Urology School of Medicine Kyungpook National University) Oh Ji Won (Department of Anatomy School of Medicine Kyungpook National University)
저널정보
한국조직공학과 재생의학회 조직공학과 재생의학 조직공학과 재생의학 제19권 제4호
발행연도
2022.8
수록면
809 - 821 (13page)
DOI
10.1007/s13770-022-00443-7

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Background: In humans, after fertilization, the zygote divides into two 2n diploid daughter blastomeres. During this division, DNA is replicated, and the remaining mutually exclusive genetic mutations in the genome of each cell are called post-zygotic variants. Using these somatic mutations, developmental lineages can be reconstructed. How these two blastomeres are contributing to the entire body is not yet identified. This study aims to evaluate the cellular contribution of two blastomeres of 2-cell embryos to the entire body in humans using post-zygotic variants based on whole genome sequencing. Methods: Tissues from different anatomical areas were obtained from five donated cadavers for use in single-cell clonal expansion and bulk target sequencing. After conducting whole genome sequencing, computational analysis was applied to find the early embryonic mutations of each clone. We developed our in-house bioinformatics pipeline, and filtered variants using strict criteria, composed of mapping quality, base quality scores, depth, soft-clipped reads, and manual inspection, resulting in the construction of embryological phylogenetic cellular trees. Results: Using our in-house pipeline for variant filtering, we could extract accurate true positive variants, and construct the embryological phylogenetic trees for each cadaver. We found that two daughter blastomeres, L1 and L2 (lineage 1 and 2, respectively), derived from the zygote, distribute unequally to the whole body at the clonal level. From bulk target sequencing data, we validated asymmetric contribution by means of the variant allele frequency of L1 and L2. The asymmetric contribution of L1 and L2 varied from person to person. Conclusion: We confirmed that there is asymmetric contribution of two daughter blastomeres from the first division of the zygote across the whole human body.

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