|
Comment |
Lhx8 ablation leads to massive autophagy of mouse oocytes associated with DNA damage. Pelosi E et al. (2018) Following proliferation of oogonia in mammals, great numbers of germ cells are discarded, primarily by apoptosis, while the remainder form primordial follicles (the ovarian reserve) that determine fertility and reproductive lifespan. More massive, rapid, and essentially total loss of oocytes, however, occurs when the transcription factor Lhx8 is ablated-though the cause and mechanism of germ cell loss from the Lhx8-/- ovaries has been unknown. We found that Lhx8-/- ovaries maintain the same number of germ cells throughout embryonic development; rapid decrease in the pool of oocytes starts shortly before birth. The loss results from activation of autophagy, which becomes overwhelming within the first postnatal week, with extracellular matrix proteins filling the space previously occupied by follicles to produce a fibrotic ovary. Associated with this process, as early as a few days before birth, Lhx8-/- oocytes failed to repair DNA damage-which normally occurs when meiosis is initiated during embryonic development; and DNA damage repair genes were down-regulated throughout the oocyte short lifespan. Based on gene expression analyses and morphological changes, we propose a model in which lineage-restricted failure of DNA repair triggers germ cell autophagy, causing premature depletion of the ovarian reserve in Lhx8-/- mice.//////////////////
|
|
Mutations |
2 mutations
Species: mouse
Mutation name: None
type: null mutation
fertility: fertile
Comment: Birk OS, et al 2000 reported that the LIM homeobox gene Lhx9 is essential for mouse gonad
formation.
During mammalian embryonic development, the ovaries and testes develop from
somatic cells of the urogenital ridges as indifferent gonads, harbouring primordial germ cells that have migrated there. After sex determination of the gonads, the testes produce testosterone and anti-Mullerian hormone which mediate male sexual differentiation, and the female developmental pathway ensues in their
absence. The authors showed that transcripts of the LIM homeobox gene Lhx9 are present in urogenital ridges of mice at embryonic day 9.5; later they localize to the
interstitial region as morphological differentiation occurs. In mice lacking Lhx9 function, germ cells migrate normally, but somatic cells of the genital ridge fail to
proliferate and a discrete gonad fails to form. In the absence of testosterone and
anti-Mullerian hormone, genetically male mice are phenotypically female. The
expression of steroidogenic factor 1 (Sf1), a nuclear receptor essential for
gonadogenesis, is reduced to minimal levels in the Lhx9-deficient genital ridge,
indicating that Lhx9 may lie upstream of Sf1 in a developmental cascade. Unlike
mice lacking other genes that mediate early stages of gonadogenesis, Lhx9 mutants
do not exhibit additional major developmental defects. Thus, LHX9 mutations may
underlie certain forms of isolated gonadal agenesis in humans.
Species: mouse
Mutation name:
type: null mutation
fertility: infertile - ovarian defect
Comment: Lhx8 ablation leads to massive autophagy of mouse oocytes associated with DNA damage. Pelosi E et al. (2018) Following proliferation of oogonia in mammals, great numbers of germ cells are discarded, primarily by apoptosis, while the remainder form primordial follicles (the ovarian reserve) that determine fertility and reproductive lifespan. More massive, rapid, and essentially total loss of oocytes, however, occurs when the transcription factor Lhx8 is ablated-though the cause and mechanism of germ cell loss from the Lhx8-/- ovaries has been unknown. We found that Lhx8-/- ovaries maintain the same number of germ cells throughout embryonic development; rapid decrease in the pool of oocytes starts shortly before birth. The loss results from activation of autophagy, which becomes overwhelming within the first postnatal week, with extracellular matrix proteins filling the space previously occupied by follicles to produce a fibrotic ovary. Associated with this process, as early as a few days before birth, Lhx8-/- oocytes failed to repair DNA damage-which normally occurs when meiosis is initiated during embryonic development; and DNA damage repair genes were down-regulated throughout the oocyte short lifespan. Based on gene expression analyses and morphological changes, we propose a model in which lineage-restricted failure of DNA repair triggers germ cell autophagy, causing premature depletion of the ovarian reserve in Lhx8-/- mice.//////////////////
|