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Literature DB >> 29443055

A Seminiferous Tubule Squash Technique for the Cytological Analysis of Spermatogenesis Using the Mouse Model.

Stephen R Wellard¹, Jessica Hopkins¹, Philip W Jordan².

Abstract

Meiotic progression in males is a process that requires the concerted action of a number of highly regulated cellular events. Errors occurring during meiosis can lead to infertility, pregnancy loss or genetic defects. Commencing at the onset of puberty and continuing throughout adulthood, continuous semi-synchronous waves of spermatocytes undergo spermatogenesis and ultimately form haploid sperm. The first wave of mouse spermatocytes undergoing meiotic initiation appear at day 10 post-partum (10 dpp) and are released into the lumen of seminiferous tubules as mature sperm at 35 dpp. Therefore, it is advantageous to utilize mice within this developmental time-window in order to obtain highly enriched populations of interest. Analysis of rare cell stages is more difficult in older mice due to the contribution of successive spermatogenic waves, which increase the diversity of the cellular populations within the tubules. The method described here is an easily implemented technique for the cytological evaluation of the cells found within the seminiferous tubules of mice, including spermatogonia, spermatocytes, and spermatids. The tubule squash technique maintains the integrity of isolated male germ cells and allows examination of cellular structures that are not easily visualized with other techniques. To demonstrate the possible applications of this tubule squash technique, spindle assembly was monitored in spermatocytes progressing through the prophase to metaphase I transition (G2/MI transition). In addition, centrosome duplication, meiotic sex chromosome inactivation (MSCI), and chromosome bouquet formation were assessed as examples of the cytological structures that can be observed using this tubule squash method. This technique can be used to pinpoint specific defects during spermatogenesis that are caused by mutation or exogenous perturbation, and thus, contributes to our molecular understanding of spermatogenesis.

Entities: Chemical Disease Gene Species

Mesh：

Year: 2018 PMID： 29443055 PMCID： PMC5912363 DOI： 10.3791/56453

Source DB: PubMed Journal: J Vis Exp ISSN： 1940-087X Impact factor: 1.355

38 in total

1. A modified cryosection method for mouse testis tissue.

Authors: X Xu; P X Xu
Journal: Tissue Cell Date: 2001-04 Impact factor: 2.466

2. Preparation, isolation and characterization of stage-specific spermatogenic cells for cellular and molecular analysis.

Authors: Noora Kotaja; Sarah Kimmins; Stefano Brancorsini; Didier Hentsch; Jean-Luc Vonesch; Irwin Davidson; Martti Parvinen; Paolo Sassone-Corsi
Journal: Nat Methods Date: 2004-12 Impact factor: 28.547

3. An early and massive wave of germinal cell apoptosis is required for the development of functional spermatogenesis.

Authors: I Rodriguez; C Ody; K Araki; I Garcia; P Vassalli
Journal: EMBO J Date: 1997-05-01 Impact factor: 11.598

4. Centrosomal association of histone macroH2A1.2 in embryonic stem cells and somatic cells.

Authors: J E Mermoud; A M Tassin; J R Pehrson; N Brockdorff
Journal: Exp Cell Res Date: 2001-08-15 Impact factor: 3.905

5. Purification, culture, and fractionation of spermatogenic cells.

Authors: A R Bellvé
Journal: Methods Enzymol Date: 1993 Impact factor: 1.600

6. Suppression of spermatogenesis by bisdichloroacetyldiamines is mediated by inhibition of testicular retinoic acid biosynthesis.

Authors: John K Amory; Charles H Muller; Jakob A Shimshoni; Nina Isoherranen; Jisun Paik; Jan S Moreb; David W Amory; Ryan Evanoff; Alex S Goldstein; Michael D Griswold
Journal: J Androl Date: 2010-08-12

7. Spermatogenesis in the immature mouse proceeds faster than in the adult.

Authors: P M Kluin; M F Kramer; D G de Rooij
Journal: Int J Androl Date: 1982-06

8. Turning a spermatogenic wave into a tsunami: synchronizing murine spermatogenesis using WIN 18,446.

Authors: Cathryn A Hogarth; Ryan Evanoff; Debra Mitchell; Travis Kent; Christopher Small; John K Amory; Michael D Griswold
Journal: Biol Reprod Date: 2013-02-14 Impact factor: 4.285

9. Previously uncharacterized histone acetyltransferases implicated in mammalian spermatogenesis.

Authors: Bruce T Lahn; Zhao Lan Tang; Jianxin Zhou; Robert J Barndt; Martti Parvinen; C David Allis; David C Page
Journal: Proc Natl Acad Sci U S A Date: 2002-06-18 Impact factor: 11.205

10. CEP63 deficiency promotes p53-dependent microcephaly and reveals a role for the centrosome in meiotic recombination.

Authors: Marko Marjanović; Carlos Sánchez-Huertas; Berta Terré; Rocío Gómez; Jan Frederik Scheel; Sarai Pacheco; Philip A Knobel; Ana Martínez-Marchal; Suvi Aivio; Lluís Palenzuela; Uwe Wolfrum; Peter J McKinnon; José A Suja; Ignasi Roig; Vincenzo Costanzo; Jens Lüders; Travis H Stracker
Journal: Nat Commun Date: 2015-07-09 Impact factor: 14.919

6 in total

A Seminiferous Tubule Squash Technique for the Cytological Analysis of Spermatogenesis Using the Mouse Model.

1. A modified cryosection method for mouse testis tissue.

2. Preparation, isolation and characterization of stage-specific spermatogenic cells for cellular and molecular analysis.

3. An early and massive wave of germinal cell apoptosis is required for the development of functional spermatogenesis.

4. Centrosomal association of histone macroH2A1.2 in embryonic stem cells and somatic cells.

5. Purification, culture, and fractionation of spermatogenic cells.

6. Suppression of spermatogenesis by bisdichloroacetyldiamines is mediated by inhibition of testicular retinoic acid biosynthesis.

7. Spermatogenesis in the immature mouse proceeds faster than in the adult.

8. Turning a spermatogenic wave into a tsunami: synchronizing murine spermatogenesis using WIN 18,446.

9. Previously uncharacterized histone acetyltransferases implicated in mammalian spermatogenesis.

10. CEP63 deficiency promotes p53-dependent microcephaly and reveals a role for the centrosome in meiotic recombination.

1. Trim41 is required to regulate chromosome axis protein dynamics and meiosis in male mice.

2. KCTD19 and its associated protein ZFP541 are independently essential for meiosis in male mice.

3. IGSF11 is required for pericentric heterochromatin dissociation during meiotic diplotene.

4. Aurora B and C kinases regulate chromosome desynapsis and segregation during mouse and human spermatogenesis.

5. Overlapping roles for PLK1 and Aurora A during meiotic centrosome biogenesis in mouse spermatocytes.

6. Depletion of SMC5/6 sensitizes male germ cells to DNA damage.