Your search keyword '"O'Bryan MK"' showing total 17 results

1. DDB1- and CUL4-associated factor 12-like protein 1 (Dcaf12l1) is not essential for male fertility in mice.

Author

Houston BJ, Lopes AM, Laan M, Nagirnaja L, O'Connor AE, Merriner DJ, Nguyen J, Punab M, Riera-Escamilla A, Krausz C, Aston KI, Conrad DF, and O'Bryan MK

Subjects

Animals, Humans, Male, Mice, Factor XII metabolism, Mice, Knockout, Sperm Motility genetics, Spermatogenesis genetics, Fertility genetics, Infertility, Male genetics, Testis

Abstract

Male infertility is a common condition affecting at least 7% of men worldwide and is often genetic in origin. Using whole exome sequencing, we recently discovered three hemizygous, likely damaging variants in DDB1- and CUL4-associated factor 12-like protein 1 (DCAF12L1) in men with azoospermia. DCAF12L1 is located on the X-chromosome and as identified by single cell sequencing studies, its expression is enriched in human testes and specifically in Sertoli cells and spermatogonia. However, very little is known about the role of DCAF12L1 in spermatogenesis, thus we generated a knockout mouse model to further explore the role of DCAF12L1 in male fertility. Knockout mice were generated using CRISPR/Cas9 technology to remove the entire coding region of Dcaf12l1 and were assessed for fertility over a broad range of ages (2-8 months of age). Despite outstanding genetic evidence in men, loss of DCAF12L1 had no discernible impact on male fertility in mice, as highlighted by breeding trials, histological assessment of the testis and epididymis, daily sperm production and evaluation of sperm motility using computer assisted methods. This disparity is likely due to the parallel evolution, and subsequent divergence, of DCAF12 family members in mice and men or the presence of compounding environmental factors in men., (Copyright © 2022 Elsevier Inc. All rights reserved.)

Published

2022

2. HENMT1 is involved in the maintenance of normal female fertility in the mouse.

Author

Hutt KJ, Lim SL, Zhang QH, Gonzalez M, O'Connor AE, Merriner DJ, Liew SH, Al-Zubaidi U, Yuen WS, Adhikari D, Robker RL, Mann JR, Carroll J, and O'Bryan MK

Subjects

Animals, Female, Gene Expression Regulation, Developmental, Infertility, Female genetics, Infertility, Female physiopathology, Methyltransferases genetics, Mice, RNA, Small Interfering genetics, Transcriptome, Fertility, Infertility, Female enzymology, Meiosis, Methyltransferases metabolism, Oocytes enzymology, Oogenesis, RNA, Small Interfering metabolism

Abstract

PIWI-interacting small RNAs (piRNAs) maintain genome stability in animal germ cells, with a predominant role in silencing transposable elements. Mutations in the piRNA pathway in the mouse uniformly lead to failed spermatogenesis and male sterility. By contrast, mutant females are fertile. In keeping with this paradigm, we previously reported male sterility and female fertility associated with loss of the enzyme HENMT1, which is responsible for stabilising piRNAs through the catalysation of 3'-terminal 2'-O-methylation. However, the Henmt1 mutant females were poor breeders, suggesting they could be subfertile. Therefore, we investigated oogenesis and female fertility in these mice in greater detail. Here, we show that mutant females indeed have a 3- to 4-fold reduction in follicle number and reduced litter sizes. In addition, meiosis-II mutant oocytes display various spindle abnormalities and have a dramatically altered transcriptome which includes a down-regulation of transcripts required for microtubule function. This down-regulation could explain the spindle defects observed with consequent reductions in litter size. We suggest these various effects on oogenesis could be exacerbated by asynapsis, an apparently universal feature of piRNA mutants of both sexes. Our findings reveal that loss of the piRNA pathway in females has significant functional consequences., (© The Author(s) 2021. Published by Oxford University Press on behalf of European Society of Human Reproduction and Embryology. All rights reserved. For permissions, please email: journals.permissions@oup.com.)

Published

2021

3. The Sertoli cell expressed gene secernin-1 (Scrn1) is dispensable for male fertility in the mouse.

Author

Houston BJ, Nagirnaja L, Merriner DJ, O'Connor AE, Okuda H, Omurtag K, Smith C, Aston KI, Conrad DF, and O'Bryan MK

Subjects

Animals, Embryo, Mammalian, Female, Infertility, Male genetics, Infertility, Male metabolism, Male, Mice, Mice, Inbred C57BL, Mice, Knockout, Nerve Tissue Proteins genetics, Pregnancy, Sertoli Cells physiology, Spermatogenesis genetics, Testis metabolism, Fertility genetics, Nerve Tissue Proteins metabolism, Sertoli Cells metabolism

Abstract

Background: Male infertility is a prevalent clinical presentation for which there is likely a strong genetic component due to the thousands of genes required for spermatogenesis. Within this study we investigated the role of the gene Scrn1 in male fertility. Scrn1 is preferentially expressed in XY gonads during the period of sex determination and in adult Sertoli cells based on single cell RNA sequencing. We investigated the expression of Scrn1 in juvenile and adult tissues and generated a knockout mouse model to test its role in male fertility., Results: Scrn1 was expressed at all ages examined in the post-natal testis; however, its expression peaked at postnatal days 7-14 and SCRN1 protein was clearly localized to Sertoli cells. Scrn1 deletion was achieved via removal of exon 3, and its loss had no effect on male fertility or sex determination. Knockout mice were capable of siring litters of equal size to wild type counterparts and generated equal numbers of sperm with comparable motility and morphology characteristics., Conclusions: Scrn1 was found to be dispensable for male fertility, but this study identifies SCRN1 as a novel marker of the Sertoli cell cytoplasm., (© 2021 American Association of Anatomists.)

Published

2021

4. The functions of CAP superfamily proteins in mammalian fertility and disease.

Author

Gaikwad AS, Hu J, Chapple DG, and O'Bryan MK

Subjects

Animals, Arabidopsis Proteins chemistry, Disease genetics, Female, Fertility genetics, Humans, Male, Mammals, Proteins chemistry, Reproduction genetics, Reproduction physiology, Seminal Plasma Proteins chemistry, Wasp Venoms chemistry, Disease etiology, Fertility physiology, Multigene Family physiology, Proteins physiology, Seminal Plasma Proteins physiology

Abstract

Background: Members of the cysteine-rich secretory proteins (CRISPS), antigen 5 (Ag5) and pathogenesis-related 1 (Pr-1) (CAP) superfamily of proteins are found across the bacterial, fungal, plant and animal kingdoms. Although many CAP superfamily proteins remain poorly characterized, over the past decade evidence has accumulated, which provides insights into the functional roles of these proteins in various processes, including fertilization, immune defence and subversion, pathogen virulence, venom toxicology and cancer biology., Objective and Rationale: The aim of this article is to summarize the current state of knowledge on CAP superfamily proteins in mammalian fertility, organismal homeostasis and disease pathogenesis., Search Methods: The scientific literature search was undertaken via PubMed database on all articles published prior to November 2019. Search terms were based on following keywords: 'CAP superfamily', 'CRISP', 'Cysteine-rich secretory proteins', 'Antigen 5', 'Pathogenesis-related 1', 'male fertility', 'CAP and CTL domain containing', 'CRISPLD1', 'CRISPLD2', 'bacterial SCP', 'ion channel regulator', 'CatSper', 'PI15', 'PI16', 'CLEC', 'PRY proteins', 'ASP proteins', 'spermatogenesis', 'epididymal maturation', 'capacitation' and 'snake CRISP'. In addition to that, reference lists of primary and review article were reviewed for additional relevant publications., Outcomes: In this review, we discuss the breadth of knowledge on CAP superfamily proteins with regards to their protein structure, biological functions and emerging significance in reproduction, health and disease. We discuss the evolution of CAP superfamily proteins from their otherwise unembellished prokaryotic predecessors into the multi-domain and neofunctionalized members found in eukaryotic organisms today. At least in part because of the rapid evolution of these proteins, many inconsistencies in nomenclature exist within the literature. As such, and in part through the use of a maximum likelihood phylogenetic analysis of the vertebrate CRISP subfamily, we have attempted to clarify this confusion, thus allowing for a comparison of orthologous protein function between species. This framework also allows the prediction of functional relevance between species based on sequence and structural conservation., Wider Implications: This review generates a picture of critical roles for CAP proteins in ion channel regulation, sterol and lipid binding and protease inhibition, and as ligands involved in the induction of multiple cellular processes., (© The Author(s) 2020. Published by Oxford University Press on behalf of the European Society of Human Reproduction and Embryology. All rights reserved. For permissions, please e-mail: journals.permission@oup.com.)

Published

2020

5. CRISP2 Is a Regulator of Multiple Aspects of Sperm Function and Male Fertility.

Author

Lim S, Kierzek M, O'Connor AE, Brenker C, Merriner DJ, Okuda H, Volpert M, Gaikwad A, Bianco D, Potter D, Prabhakar R, Strünker T, and O'Bryan MK

Subjects

Acrosome Reaction physiology, Animals, Cell Adhesion Molecules, Infertility, Male genetics, Male, Membrane Proteins genetics, Mice, Mice, Knockout, Sperm Motility physiology, Fertility physiology, Infertility, Male metabolism, Membrane Proteins metabolism, Spermatogenesis physiology, Spermatozoa metabolism

Abstract

The cysteine-rich secretory proteins (CRISPs) are a group of proteins that show a pronounced expression biased to the male reproductive tract. Although sperm encounter CRISPs at virtually all phases of sperm development and maturation, CRISP2 is the sole CRISP produced during spermatogenesis, wherein it is incorporated into the developing sperm head and tail. In this study we tested the necessity for CRISP2 in male fertility using Crisp2 loss-of-function mouse models. In doing so, we revealed a role for CRISP2 in establishing the ability of sperm to undergo the acrosome reaction and in establishing a normal flagellum waveform. Crisp2-deficient sperm possess a stiff midpiece and are thus unable to manifest the rapid form of progressive motility seen in wild type sperm. As a consequence, Crisp2-deficient males are subfertile. Furthermore, a yeast two-hybrid screen and immunoprecipitation studies reveal that CRISP2 can bind to the CATSPER1 subunit of the Catsper ion channel, which is necessary for normal sperm motility. Collectively, these data define CRISP2 as a determinant of male fertility and explain previous clinical associations between human CRISP2 expression and fertility., (Copyright © 2019 Endocrine Society.)

Published

2019

6. Changes in sperm methylation profile: a potential cause of infertility and a handle to monitor improvements in genetic and lifestyle interactions.

Author

O'Bryan MK and Lane M

Subjects

Female, Humans, Male, Pregnancy, DNA Methylation, Epigenesis, Genetic, Fertility genetics, Infertility, Male genetics, Spermatozoa metabolism

Published

2016

7. Contribution of the two genes encoding histone variant h3.3 to viability and fertility in mice.

Author

Tang MC, Jacobs SA, Mattiske DM, Soh YM, Graham AN, Tran A, Lim SL, Hudson DF, Kalitsis P, O'Bryan MK, Wong LH, and Mann JR

Subjects

Animals, DNA Replication genetics, Female, Fetus, Male, Meiosis genetics, Mice, Oocytes growth & development, Spermatocytes growth & development, Spermatocytes pathology, Spermatozoa growth & development, Spermatozoa pathology, Zygote, Cell Survival genetics, Chromatin genetics, Fertility genetics, Histones genetics, Oogenesis

Abstract

Histones package DNA and regulate epigenetic states. For the latter, probably the most important histone is H3. Mammals have three near-identical H3 isoforms: canonical H3.1 and H3.2, and the replication-independent variant H3.3. This variant can accumulate in slowly dividing somatic cells, replacing canonical H3. Some replication-independent histones, through their ability to incorporate outside S-phase, are functionally important in the very slowly dividing mammalian germ line. Much remains to be learned of H3.3 functions in germ cell development. Histone H3.3 presents a unique genetic paradigm in that two conventional intron-containing genes encode the identical protein. Here, we present a comprehensive analysis of the developmental effects of null mutations in each of these genes. H3f3a mutants were viable to adulthood. Females were fertile, while males were subfertile with dysmorphic spermatozoa. H3f3b mutants were growth-deficient, dying at birth. H3f3b heterozygotes were also growth-deficient, with males being sterile because of arrest of round spermatids. This sterility was not accompanied by abnormalities in sex chromosome inactivation in meiosis I. Conditional ablation of H3f3b at the beginning of folliculogenesis resulted in zygote cleavage failure, establishing H3f3b as a maternal-effect gene, and revealing a requirement for H3.3 in the first mitosis. Simultaneous ablation of H3f3a and H3f3b in folliculogenesis resulted in early primary oocyte death, demonstrating a crucial role for H3.3 in oogenesis. These findings reveal a heavy reliance on H3.3 for growth, gametogenesis, and fertilization, identifying developmental processes that are particularly susceptible to H3.3 deficiency. They also reveal partial redundancy in function of H3f3a and H3f3b, with the latter gene being generally the most important.

Published

2015

8. KATNB1 in the human testis and its genetic variants in fertile and oligoasthenoteratozoospermic infertile men.

Author

O'Donnell L, McLachlan RI, Merriner DJ, O'Bryan MK, and Jamsai D

Subjects

Adenosine Triphosphatases chemistry, Amino Acid Sequence, Animals, Genetic Variation, Humans, Katanin, Male, Molecular Sequence Data, Sequence Homology, Amino Acid, Adenosine Triphosphatases genetics, Fertility, Infertility, Male metabolism, Testis metabolism

Abstract

Oligoasthenoteratozoospermia (OAT) is a phenotype frequently observed in infertile men, and is defined by low spermatozoa number, abnormal spermatozoa morphology and poor motility. We previously showed that a mutation in the Katnb1 gene in mice causes infertility because of OAT. The KATNB1 gene encodes an accessory subunit of the katanin microtubule-severing enzyme complex; this accessory subunit is thought to modulate microtubule-severing location and activity. We hypothesized that KATNB1 may play a role in human spermatogenesis and that genetic variants in KATNB1 could be associated with OAT in humans. Using immunostaining, we defined the localization of the KATNB1 protein in human testes. KATNB1 was present during spermatid development, and in particular localized to the microtubules of the manchette, a structure required for sperm head shaping. To assess a potential association between genetic variants in the KATNB1 gene and infertile men with OAT, we performed direct sequencing of genomic DNA samples from 100 OAT infertile and 100 proven fertile men. Thirty-seven KATNB1 variants were observed, five of which had not previously been described. Ten variants were present only in OAT men, however, statistical analysis did not reveal a significant association with fertility status. Our results suggest that variants in the KATNB1 gene are not commonly associated with OAT infertility in Australian men., (© 2014 American Society of Andrology and European Academy of Andrology.)

Published

2014

9. Genetic variants in the RABL2A gene in fertile and oligoasthenospermic infertile men.

Author

Jamsai D, Lo JC, McLachlan RI, and O'Bryan MK

Subjects

Computational Biology, Exons, Gene Frequency, Genetic Association Studies, Genetic Predisposition to Disease, High-Throughput Nucleotide Sequencing, Humans, Infertility, Male physiopathology, Introns, Male, Phenotype, Risk Factors, Untranslated Regions, Victoria, Fertility genetics, Genetic Variation, Infertility, Male genetics, rab GTP-Binding Proteins genetics

Abstract

Objective: To define RABL2A localization in human sperm and to assess any potential association between RABL2A variants and male infertility associated with oligoasthenospermia., Design: Genetic association study., Setting: Public university., Patient(s): Australian men: 110 oligoasthenospermic infertile and 105 proven fertile., Intervention(s): Human semen samples processed by immunostaining with high-throughput-sequencing platform to screen the entire protein-coding and flanking exon/intron regions of the RABL2A gene., Main Outcome Measure(s): Presence of RABL2A in human sperm and frequencies of RABL2A genetic variants in fertile and infertile men., Result(s): RABL2A localization in sperm was highly conserved between mouse and human, being localized to the tail. Direct DNA sequencing revealed 23 RABL2A genetic variants, including 16 intronic, 6 untranslated region (UTR), and one exonic missense variants. Of these, eight variants have not been previously reported. Although the majority of these variants showed no significant association with fertility status, allelic frequency of the intronic variant 114391996 delC was significantly increased in oligoasthenospermic men. Bioinformatics analysis suggested that the 114391996 delC allele would alter the splicing of RABL2A pre-mRNA., Conclusion(s): Our data suggest the 114391996 delC allele in the RABL2A gene may act as a risk factor for oligoasthenospermic infertility in Australian men., (Copyright © 2014 American Society for Reproductive Medicine. Published by Elsevier Inc. All rights reserved.)

Published

2014

10. Genetic variants in the human glucocorticoid-induced leucine zipper (GILZ) gene in fertile and infertile men.

Author

Jamsai D, Grealy A, Stahl PJ, Schlegel PN, McLachlan RI, Morand E, and O'Bryan MK

Subjects

Humans, Male, Fertility genetics, Genetic Variation, Infertility, Male genetics, Transcription Factors genetics

Abstract

Sertoli cell only (SCO) syndrome is the predominant histology for men with non-obstructive azoospermia (NOA) and is usually of unexplained aetiology. Studies in mouse models indicated that the X-linked gene glucocorticoid-induced leucine zipper (GILZ) is essential for survival and differentiation of spermatogonia, and meiosis. GILZ deficiency results in a rapid and progressive loss of germ cells with SCO tubules and sterility in adults. The role of GILZ in human fertility has not been examined. Here we show that GILZ is localized to spermatogonia and spermatocytes in the human testis in a pattern analogous to that seen in mice. To assess the potential for an association between GILZ variants and human infertility, we sequenced the entire protein-coding regions of the GILZ gene in 65 SCO and 87 fertile Australian men. We identified six genetic variants, three of which had not been reported previously. Three variants, 107018665 G>A, 107018485 C>G and 106959283 C>T, were found at a low frequency only in SCO men. Although none of the identified variants changed the protein code, sequence analysis indicated that two variants, 107018665 G>A and 107018485 C>G, would completely abolish the exonic splicing enhancer (ESE)-binding motifs for the splicing factors SF2/ASF and SC35 respectively. This result prompted an assessment of whether these two variants were associated with male infertility in a separate population of men. We used a PCR-based SNP detection approach to screen an additional 52 NOA and 153 fertile Australian men, and 86 SCO and 54 fertile American men. None of these men carried either of these two variants. The cumulative allelic frequency of these variants is less than 1% in SCO men and no association with fertility status was observed. Our study suggests that GILZ variants are not common causes of SCO and NOA in Australian or American men., (© 2013 American Society of Andrology and European Academy of Andrology.)

Published

2013

11. Genetic variants in the ETV5 gene in fertile and infertile men with nonobstructive azoospermia associated with Sertoli cell-only syndrome.

Author

O'Bryan MK, Grealy A, Stahl PJ, Schlegel PN, McLachlan RI, and Jamsai D

Subjects

Adult, Alternative Splicing genetics, Australia epidemiology, Azoospermia epidemiology, Azoospermia pathology, Base Sequence, Genetic Predisposition to Disease epidemiology, Genetic Predisposition to Disease genetics, Humans, Male, Molecular Sequence Data, RNA Precursors genetics, Risk Factors, Sertoli Cell-Only Syndrome epidemiology, Sertoli Cell-Only Syndrome pathology, Spermatogonia pathology, Spermatogonia physiology, Testis pathology, Testis physiology, Azoospermia genetics, DNA-Binding Proteins genetics, Fertility genetics, Genetic Variation genetics, Sertoli Cell-Only Syndrome genetics, Transcription Factors genetics

Abstract

Objective: To assess the association between genetic variants in the ETV5 gene with nonobstructive azoospermia (NOA) associated with Sertoli cell-only (SCO) syndrome., Design: Genetic association study., Setting: University., Patient(s): Australian men (65 SCO, 53 NOA, and 242 fertile men) and American men (86 SCO and 54 fertile men)., Intervention(s): Paraffin-embedded human testicular tissue was sectioned and processed for immunofluorescence. Direct DNA sequencing and polymerase chain reaction-based SNP detection were performed to define genetic variants in the ETV5 gene., Main Outcome Measure(s): The localization of ETV5 in the human testis and the presence of ETV5 genetic variants in fertile and infertile men., Result(s): ETV5 is localized to the cytoplasm and nucleus of Sertoli and germ cells in adult human testes. We identified six previously reported and six new genetic variants in the ETV5 gene. Of these, the allele frequency of the homozygous +48845 G>T (TT allele) variant was significantly higher in the SCO and NOA Australian men compared with fertile men., Conclusion(s): The homozygous +48845 G>T (TT allele) variant confers a higher risk for male infertility associated with NOA and SCO in Australian men., (Copyright © 2012 American Society for Reproductive Medicine. All rights reserved.)

Published

2012

12. The role of cysteine-rich secretory proteins in male fertility.

Author

Koppers AJ, Reddy T, and O'Bryan MK

Subjects

Animals, Epididymis metabolism, Male, Fertility physiology, Seminal Plasma Proteins metabolism, Spermatogenesis physiology, Spermatozoa metabolism

Abstract

The cysteine-rich secretory proteins (CRISPs) are a subgroup of the CRISP, antigen 5 and Pr-1 (CAP) protein superfamily, and are found only in vertebrates. They show a strong expression bias to the mammalian male reproductive tract and the venom of poisonous reptiles. Within the male reproductive tract CRISPs have been implicated in many aspects of male germ cell biology spanning haploid germ cell development, epididymal maturation, capacitation, motility and the actual processes of fertilization. At a structural level, CRISPs are composed of two domains, a CAP domain, which has been implicated in cell-cell adhesion, and a CRISP domain, which has been shown to regulate several classes of ion channels across multiple species. Herein, we will review the current literature on the role of CRISPs in male fertility, and by inference to related non-mammalian protein, infer potential biochemical functions.

Published

2011

13. Mouse models in male fertility research.

Author

Jamsai D and O'Bryan MK

Subjects

Animals, Humans, Infertility, Male genetics, Male, Mice, Mice, Transgenic, Disease Models, Animal, Fertility physiology, Infertility, Male physiopathology, Spermatogenesis physiology

Abstract

Limited knowledge of the genetic causes of male infertility has resulted in few treatment and targeted therapeutic options. Although the ideal approach to identify infertility causing mutations is to conduct studies in the human population, this approach has progressed slowly due to the limitations described herein. Given the complexity of male fertility, the entire process cannot be modeled in vitro. As such, animal models, in particular mouse models, provide a valuable alternative for gene identification and experimentation. Since the introduction of molecular biology and recent advances in animal model production, there has been a substantial acceleration in the identification and characterization of genes associated with many diseases, including infertility. Three major types of mouse models are commonly used in biomedical research, including knockout/knockin/gene-trapped, transgenic and chemical-induced point mutant mice. Using these mouse models, over 400 genes essential for male fertility have been revealed. It has, however, been estimated that thousands of genes are involved in the regulation of the complex process of male fertility, as many such genes remain to be characterized. The current review is by no means a comprehensive list of these mouse models, rather it contains examples of how mouse models have advanced our knowledge of post-natal germ cell development and male fertility regulation.

Published

2011

14. Genome-wide ENU mutagenesis for the discovery of novel male fertility regulators.

Author

Jamsai D and O'Bryan MK

Subjects

Animals, Fertility genetics, Male, Mice, Mice, Transgenic, Ethylnitrosourea toxicity, Fertility drug effects, Mutagens toxicity

Abstract

The completion of genome sequencing projects has provided an extensive knowledge of the contents of the genomes of human, mouse, and many other organisms. Despite this, the function of most of the estimated 25,000 human genes remains largely unknown. Attention has now turned to elucidating gene function and identifying biological pathways that contribute to human diseases, including male infertility. Our understanding of the genetic regulation of male fertility has been accelerated through the use of genetically modified mouse models including knockout, knock-in, gene-trapped, and transgenic mice. Such reverse genetic approaches however, require some fore-knowledge of a gene's function and, as such, bias against the discovery of completely novel genes and biological pathways. To facilitate high throughput gene discovery, genome-wide mouse mutagenesis via the use of a potent chemical mutagen, N-ethyl-N-nitrosourea (ENU), has been developed over the past decade. This forward genetic, or phenotype-driven, approach relies upon observing a phenotype first, then subsequently defining the underlining genetic defect. Mutations are randomly introduced into the mouse genome via ENU exposure. Through a controlled breeding scheme, mutations causing a phenotype of interest (e.g., male infertility) are then identified by linkage analysis and candidate gene sequencing. This approach allows for the possibility of revealing comprehensive phenotype-genotype relationships for a range of genes and pathways i.e. in addition to null alleles, mice containing partial loss of function or gain-of-function mutations, can be recovered. Such point mutations are likely to be more reflective of those that occur within the human population. Many research groups have successfully used this approach to generate infertile mouse lines and some novel male fertility genes have been revealed. In this review, we focus on the utility of ENU mutagenesis for the discovery of novel male fertility regulators.

Published

2010

15. Mouse models as tools in fertility research and male-based contraceptive development.

Author

Jamsai D and O'Bryan MK

Subjects

Animals, Humans, Male, Mice, Knockout, Mice, Transgenic, Mutagenesis, Point Mutation, Contraceptive Agents, Male pharmacology, Fertility drug effects, Fertility genetics, Mice physiology

Abstract

The production of functional spermatozoa is a complex process requiring the coordinated expression of thousands of genes. It is likely that the intricate nature of these interactions contributes to the large number of idiopathic male infertility cases seen in humans. Conversely, the complexity of the highly regulated and interconnected processes of spermatogenesis and posttesticular sperm maturation events offers opportunities for the development of male-based contraceptive targets. The recent advances in genetic manipulation technologies and the completion of the human and mouse genome sequencing programs have provided scientists with sophisticated ways to generate mouse models for the study of basic biological mechanisms, in order to understand disease pathology and develop novel therapeutic approaches. The three common types of mouse model used for medical research are transgenic, knockout/knockin, and chemical-induced point mutant mice. Each type has relative strengths and weaknesses with respect to its fidelity to the disease processes in humans. In this chapter, we focus on the utility of the different types of mouse model in obtaining a better understanding of the mechanisms that control spermatogenesis and developing male-based contraceptive regimens.

Published

2010

16. Sox8 is a critical regulator of adult Sertoli cell function and male fertility.

Author

O'Bryan MK, Takada S, Kennedy CL, Scott G, Harada S, Ray MK, Dai Q, Wilhelm D, de Kretser DM, Eddy EM, Koopman P, and Mishina Y

Subjects

Animals, DNA-Binding Proteins deficiency, DNA-Binding Proteins genetics, Exons, Gene Deletion, Genotype, Male, Mice embryology, Mice, Knockout, Mice, Transgenic, Polymerase Chain Reaction, Restriction Mapping, SOXE Transcription Factors, Testis cytology, Testis embryology, Testis physiology, Transcription Factors deficiency, Transcription Factors genetics, DNA-Binding Proteins physiology, Fertility physiology, Mice genetics, Sertoli Cells physiology, Transcription Factors physiology

Abstract

Sox8 encodes a high-mobility group transcription factor that is widely expressed during development. Sox8, -9 and -10 form group E of the Sox gene family which has been implicated in several human developmental disorders. In contrast to other SoxE genes, the role of Sox8 is unclear and Sox8 mouse mutants reportedly showed only idiopathic weight loss and reduced bone density. The careful analysis of our Sox8 null mice, however, revealed a progressive male infertility phenotype. Sox8 null males only sporadically produced litters of reduced size at young ages. We have shown that SOX8 protein is a product of adult Sertoli cells and its elimination results in an age-dependent deregulation of spermatogenesis, characterized by sloughing of spermatocytes and round spermatids, spermiation failure and a progressive disorganization of the spermatogenic cycle, which resulted in the inappropriate placement and juxtaposition of germ cell types within the epithelium. Those sperm that did enter the epididymides displayed abnormal motility. These data show that SOX8 is a critical regulator of adult Sertoli cell function and is required for both its cytoarchitectural and paracrine interactions with germ cells.

Published

2008

17. A repository of ENU mutant mouse lines and their potential for male fertility research.

Author

Kennedy CL, O'Connor AE, Sanchez-Partida LG, Holland MK, Goodnow CC, de Kretser DM, and O'Bryan MK

Subjects

Activins, Animals, Apoptosis, Crosses, Genetic, Female, Fertility drug effects, Fertility genetics, Follicle Stimulating Hormone blood, Male, Mice, Mice, Mutant Strains, Mutagenesis, Mutagens, Organ Size, Semen Preservation, Testis anatomy & histology, Testis drug effects, Ethylnitrosourea toxicity, Fertility physiology

Abstract

Many of the proteins and their encoding genes involved in spermatogenesis are unknown, making the specific diagnosis and treatment of infertility in males difficult and highlighting the importance of identifying new genes that are involved in spermatogenesis. Through genome-wide chemical mutagenesis using N-ethyl-N-nitrosourea (ENU) and a three-generation breeding scheme to isolate recessive mutations, we have identified mouse lines with a range of abnormalities relevant to human male fertility. Abnormal phenotypes included hypospermatogenesis, Sertoli cell-only (SCO) seminiferous tubules, germ-cell arrest and abnormal spermiogenesis and were accompanied, in some, with abnormal serum levels of reproductive hormones. In total, from 65 mouse lines, 14 showed a reproductive phenotype consistent with a recessive mutation. This study shows that it is feasible to use ENU mutagenesis as an effective and rapid means of generating mouse models relevant to furthering our understanding of human male infertility. Spermatozoa and genomic DNA from all mouse lines, including those with abnormal reproductive tract parameters, have been cryopreserved for the regeneration of lines as required. This repository will form a valuable resource for the identification and analysis of key regulators of multiple aspects of male fertility.

Published

2005