Publications by authors named "Victor A Ruthig"

Selective and controlled expansion of endogenous β-cells has been pursued as a potential therapy for diabetes. Ideally, such therapies would preserve feedback control of β-cell proliferation to avoid excessive β-cell expansion. Here, we identified a regulator of β-cell proliferation whose inactivation results in controlled β-cell expansion: the protein deacetylase Sirtuin 2 (SIRT2).

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  • The Y-linked zinc finger gene ZFY is crucial for fertility in eutherian species and plays multiple roles in mouse spermatogenesis.
  • Research on mouse homologues Zfy1 and Zfy2 showed that Zfy regulates processes like chromosome pairing and spermiogenesis, and it's essential for successful meiosis and fertility.
  • Mice lacking both Zfy homologues are infertile due to severe sperm development defects, highlighting the gene's importance and its implications for understanding human fertility-related genetic variations.
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  • DND1 plays a crucial role in preserving germ cell identity; its dysfunction leads to abnormal differentiation, resulting in teratomas in mice or somatic replacements in zebrafish.
  • In a study using a knock-in mouse model (Dnd1GFP), two populations of male germ cells were identified during their resting phase, with one group expressing low levels of DND1-GFP and another group showing high levels.
  • RNA sequencing and immunoprecipitation revealed that DND1-GFP-hi cells have significantly higher Dnd1 transcript levels and interact with various epigenetic and translational regulators, suggesting a complex network managed by DND1 essential for germ cell function.
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Genitourinary development is a delicately orchestrated process that begins in the embryo. Once complete, the genitourinary system is a collection of functionally disparate organs spread throughout the abdominal and pelvic regions. These distinct organs are interconnected through an elaborate duct system which aggregates the organs' products to a common exit point.

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Since their initial description by Enrico Sertoli in 1865, Sertoli cells have continued to enchant testis biologists. Testis size and germ cell carrying capacity are intimately tied to Sertoli cell number and function. One critical Sertoli cell function is signaling from Sertoli cells to germ cells as part of regulation of the spermatogenic cycle.

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In vertebrates, the RNA-binding protein (RBP) dead end 1 (DND1) is essential for primordial germ cell (PGC) survival and maintenance of cell identity. In multiple species, Dnd1 loss or mutation leads to severe PGC loss soon after specification or, in some species, germ cell transformation to somatic lineages. Our investigations into the role of DND1 in PGC specification and differentiation have been limited by the absence of an available antibody.

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The adult spermatogonial stem cell population arises from pluripotent primordial germ cells (PGCs) that enter the fetal testis around embryonic day (E)10.5. PGCs undergo rapid mitotic proliferation, then enter prolonged cell cycle arrest (G1/G0), during which they transition to pro-spermatogonia.

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  • Mice with deletions in the Y-chromosome's long arm (NPYq) experience increasing sperm defects and fertility issues that correlate with the size of the deletion.
  • A gene knockdown (sh367 Sly-KD) mimics some fertility issues seen in NPYq deletion mutants but is less severe, possibly due to incomplete gene suppression or involvement of other genes.
  • Research using a specific anti-SLY antibody revealed that SLY1/2 protein levels decreased with larger deletions, and adding transgenes improved SLY expression but did not fix the fertility defects, suggesting that other genes in the NPYq region also play a role in infertility.
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The male urogenital system represents a morphologically complex region that arises from a common embryological origin. However, it is typically studied separately as the excretory system is dissected with the posterior wall of the abdomen while the reproductive features are exposed with the pelvis and perineum dissection. Additionally, the reproductive structures are typically dissected following pelvic and perineal hemisection obviating a comprehensive and holistic examination.

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We recently investigated mice with Y chromosome gene contribution limited to two, one, or no Y chromosome genes in respect to their ability to produce haploid round spermatids and live offspring following round spermatid injection. Here we explored the normalcy of germ cells and Sertoli cells within seminiferous tubules, and the interstitial tissue of the testis in these mice. We performed quantitative analysis of spermatogenesis and interstitial tissue on Periodic acid-Schiff and hematoxylin-stained mouse testis sections.

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The mammalian Y chromosome is considered a symbol of maleness, as it encodes a gene driving male sex determination, Sry, as well as a battery of other genes important for male reproduction. We previously demonstrated in the mouse that successful assisted reproduction can be achieved when the Y gene contribution is limited to only two genes, Sry and spermatogonial proliferation factor Eif2s3y. Here, we replaced Sry by transgenic activation of its downstream target Sox9, and Eif2s3y, by transgenic overexpression of its X chromosome-encoded homolog Eif2s3x.

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The Y chromosome gene Sry is responsible for sex determination in mammals and initiates a cascade of events that direct differentiation of bipotential genital ridges toward male-specific fate. Sox9 is an autosomal gene and a primary downstream target of SRY. The activation of Sox9 in the absence of Sry is sufficient for initiation of male-specific sex determination.

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