Role of Deoxyribonucleic Acid Polymerase ε in Spermatogenesis in Mice1

Kamel, Dia; Mackey, Zachary B.; Sjöblom, Tiina; Walter, Christi A.; McCarrey, John R.; Uitto, Lahja; Palosaari, Heidi; Lähdetie, Jaana; Tomkinson, Alan E.; Syväoja, Juhani E.

doi:10.1095/biolreprod57.6.1367

Cited by 27 publications

(18 citation statements)

References 44 publications

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“…Haploid cells lacked detectable PCNA reactivity as well as Sertoli cells (not shown) in agreement with published observations (Kamel et al, 1997). Negative control sections where primary antibody was replaced by mouse IgG remained unstained ( Fig.…”

Section: Expression Of Mouse Kin17 Gene During Testicular Developmentsupporting

confidence: 91%

KIN17 encodes an RNA-binding protein and is expressed during mouse spermatogenesis

Pinon‐Lataillade

Masson

Bernardino-Sgherri

et al. 2004

Journal of Cell Science

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Genotoxic agents deform DNA structure thus eliciting a complex genetic response allowing recovery and cell survival. The Kin17 gene is up-regulated during this response. This gene encodes a conserved nuclear protein that shares a DNA-binding domain with the bacterial RecA protein. The KIN17 protein binds DNA and displays enhanced expression levels in proliferating cultured cells, suggesting a role in nuclear metabolism. We investigated this by studying the expression profile of KIN17 protein during mouse spermatogenesis. As expected, the expression level of Kin17 is higher in proliferating than in differentiated cells. KIN17 is selectively extracted from this tissue by detergents and a fraction was tightly associated with the nuclear matrix. Germinal cells ubiquitously express Kin17 and the protein is located mainly in the nucleus except in elongated spermatids where cytoplasmic staining is also observed. Sertoli and germ cells that are no longer mitotically active express KIN17, suggesting a general role in all testicular cell types. In adult testis a significant proportion of KIN17 co-purifies with polyadenylated RNA. KIN17 directly binds RNA, preferentially poly(G) and poly(U) homopolymers. These results together with the identification of KIN17 as a component of the human spliceosome indicate that this protein may participate in RNA processing.

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Section: Expression Of Mouse Kin17 Gene During Testicular Developmentsupporting

confidence: 91%

KIN17 encodes an RNA-binding protein and is expressed during mouse spermatogenesis

Pinon‐Lataillade

Masson

Bernardino-Sgherri

et al. 2004

Journal of Cell Science

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show abstract

“…PCNA, involved in DNA replication and repair, also prominently expressed in the nuclei of spermatogonia and primary spermatocytes (Chapman & Wolgemuth 1994, Kamel et al 1997, Steger et al 1998, Bar-Shira Maymon et al 2003. DAZL that stains intermediate and B type spermatogonia as well as preleptotene and pachytene spermatocytes (Saunders et al 2003).…”

Section: Discussionmentioning

confidence: 99%

Dexrazoxane exacerbates doxorubicin-induced testicular toxicity

Levi¹,

Tzabari²,

Savion³

et al. 2015

Reproduction

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Infertility induced by anti-cancer treatments pose a major concern for cancer survivors. Doxorubicin (DXR) has been previously shown to exert toxic effects on the testicular germinal epithelium. Based upon the cardioprotective traits of dexrazoxane (DEX), we studied its potential effect in reducing DXR-induced testicular toxicity. Male mice were injected with 5 mg/kg DXR, 100 mg/kg DEX, combination of both or saline (control) and sacrificed either 1, 3 or 6 months later. Testes were excised and further processed. Glutathione and apoptosis assays were performed to determine oxidative stress. Immunohistochemistry and confocal microscopy were used to study the effects of the drugs on testicular histology and on spermatogonial reserve. DXR and the combined treatment induced a striking decline in testicular weight. DEX prevented DXR-induced oxidative stress, but enhanced DXR-induced apoptosis within the testes. Furthermore, the combined treatment depleted the spermatogonial reserve after 1 month, with impaired recovery at 3 and 6 months post-treatment. This resulted in compromised sperm parameters, testicular and epididymal weights as well as significantly reduced sperm motility, all of which were more severe than those observed in DXR-treated mice. The activity of DEX in the testis may differ from its activity in cardiomyocytes. Adding DEX to DXR exacerbates DXR-induced testicular toxicity. Reproduction (2015) 150 357-366

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“…Mitotic and DNA metabolic activities change throughout the stages of gametogenesis (Figure 1b). Many replication, repair or recombination genes show altered or specialized expression during gametogenesis [4][5][6][7][8][9]. If expansions occur during replication, the larger number of mitotic divisions in male gametogenesis could explain the paternal bias for HD mutation.…”

Section: Expansionmentioning

confidence: 99%

“…Mouse-strain-specific differences might also account for variable murine mutation patterns: unsuspected mutations in repair genes within the supposed wild-type embryonic stem cells, such as those occurring in the polymerase iota (pol i) gene in the 129-derived strains [18], might unknowingly contribute to repeat instability. Importantly, high levels of the error-prone DNA polymerases i, k, l, h and b, as well as pol e, are present in mouse testes at various stages of spermatogenesis, before, during and after meiosis, and, in some cases, in round spermatids ( [8,9] and Refs therein). Outside of mitotic spermatogonia, the replicative polymerases a and d are present at higher levels coincident with meiotic DNA synthesis ( [8] and Refs therein).…”

Section: Cag Expansions In Germ Cells Of Hd Patientsmentioning

confidence: 99%

“…Importantly, high levels of the error-prone DNA polymerases i, k, l, h and b, as well as pol e, are present in mouse testes at various stages of spermatogenesis, before, during and after meiosis, and, in some cases, in round spermatids ( [8,9] and Refs therein). Outside of mitotic spermatogonia, the replicative polymerases a and d are present at higher levels coincident with meiotic DNA synthesis ( [8] and Refs therein). Strain-specific defects in polymerases or other repair genes might influence the interpretation of transmitted or somatic instabilities observed in transgenic mice.…”

Section: Cag Expansions In Germ Cells Of Hd Patientsmentioning

confidence: 99%

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