| Literature DB >> 32699838 |
Mariusz Z Ratajczak1, Alison Domingues1, Suman Suman1, Alex R Straughn2, Sham S Kakar1,2, Malwina Suszynska1.
Abstract
Evidence has accumulated that postnatal tissues contain developmentally early stem cells that remain in a dormant state as well as stem cells that are more proliferative, supplying tissue-specific progenitor cells and thus playing a more active role in the turnover of adult tissues. The most primitive, dormant, postnatal tissue-derived stem cells, called very small embryonic like stem cells (VSELs), are regulated by epigenetic changes in the expression of certain parentally imprinted genes, a molecular phenomenon previously described for maintaining primordial germ cells (PGCs) in a quiescent state. Specifically, they show erasure of parental imprinting at the Igf2-H19 locus, which keeps them in a quiescent state in a similar manner as migrating PGCs. To date, the presence of these cells in adult postnatal tissues have been demonstrated by at least 25 independent laboratories. We envision that similar changes in expression of parentally imprinted genes may also play a role in the quiescence of dormant VSELs present in other non-hematopoietic tissues. Recent data indicate that VSELs expand in vivo and in vitro after reestablishment of somatic imprinting at the Igf2-H19 locus by nicotinamide treatment in response to stimulation by pituitary gonadotrophins (follicle stimulating factor, luteinizing hormone and prolactin) and gonadal androgens and estrogens. These cells could be also successfully expanded ex vivo in the presence of the small molecule UM177.Entities:
Keywords: Adult stem cells; Igf2–H19 locus; imprinted genes; primordial germ cells; stem cell quiescence; tissue regeneration; tumorigenesis
Year: 2019 PMID: 32699838 PMCID: PMC7375353
Source DB: PubMed Journal: Proc Stem Cell Res Oncog ISSN: 2641-5070