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Spermatogonial stem cells (A Basic Concept)

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Title: Spermatogonial stem cells (A Basic Concept) Author: Jayanti Tokas, Rubina Begum, Shalini Jain and Hariom Yadav Last modified by: Eugene Created Date – PowerPoint PPT presentation

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Title: Spermatogonial stem cells (A Basic Concept)


1
Spermatogonial stem cells
(A Basic Concept)
Jayanti Tokas1, Rubina Begum1, Shalini Jain2 and
Hariom Yadav2 Department of Biotechnology, JMIT,
Radaur, India NIDDK, National Institutes of
Health, Bethesda, MD 20892, USA
2
  • Spermatogenesis is the process of germ cells
    proliferation and differentiation within the
    seminiferous tubules of the testes leading to
    haploid, free swimming spermatozoa.
  • Spermatogonial stem cells (present in the
    seminiferous tubules) form the basis of
    spermatogenesis.

3
  • Stem cells are characterized according to the
    tissue from which the cells are derived.
  • Embryonic stem cells
  • Adult stem cells
  • Amongst the adult stem cells, the two best
    defined systems are
  • Spermatogenesis (Spermatogonial
    stem cells, SSC)
  • Haematopoesis (Haematopoeitic
    stem cells, HSC)

4
  • Spermatogonial Stem cells (SSCs)
  • (defined by their functions)
  • Self-renewal - ability to go through numerous
    cell divisions while maintaining the
    undifferentiated state.
  • Multipotent - capacity to differentiate into any
    type of mature cell.

5
  • SSCs are the only adult stem cells that transmit
    genetic information to next generation
  • These are the eternal germ cells present from
    birth to death
  • SSC self renew and produce daughter cells that
    differentiate into spermatozoa.
  • Reside within the basal layer of seminiferous
    tubules of the testes.
  • Maintain spermatogenesis throughout life in males
    by proliferation and differentiation.

6
Fate of the spermatogonial stem cells
Type A spermatogonia
Renewal
Differentiation
Apoptosis
Type B spermatogonia
Cell death
Type A spermatogonia
7
ESTABLISHMENT OF MALE GERM LINE
8
1. Migration of primordial germ cells to
allantois region
Extra embryonic ectoderm
Epiblast
Visceral endoderm
9
2. Migration of PGCs endoderm
Allantois
PGCs
10
3. Migration of PGCs into gonad
Prenatal PGCs associate with sex cords and
secondary sex cords become seminiferous tubules.
11
  • Primordial Germ Cells differentiate to become
    gonocytes
  • Proliferate
  • Mitotic arrest until birth
  • (depending on species)

undergo
Rodents around birth Bulls 4-8 weeks of
age Boars 5-15 days of age Humans 2 yr
Gonocytes can differentiate into spermatogonial
stem cells or spermatogonia
12
After birth gonocytes
Resume mitosis Migrate to
basement membrane
Differentiate into type Ao spermatogonia
Spermatogonial stem cells originate from PGC at
7.5 days p.c.
13
Spermatogonial stem cells present in the testis
Niche - subset of tissue cells and extracellular
substrates that can indefinitely house one or
more stem cells and control their self-renewal
and progeny production in vivo.
14
Identification of spermatogonial stem cells
  • Until 1977 Isolation
  • Bovine serum albumin gradient and velocity
    sedimentation (90 purity)
  • 1990- Kit ligand/c-Kit receptor
  • Growth factor- produced by Sertoli cells
  • Regulate the growth of the spermatogonia
  • Used as marker for A spermatogonia

15
  • Stages of cell division can be used to
    distinguish between stem cells and
    differentiating cells
  • SSCs activities can be identified by the
    formation of colonies
  • Surface phenotype for identification
  • Thy-1- unique marker for mouse and rat SSC
  • Surface phenotype - MHC-1 Thy-1 c-Kit,
    av-integrin these markers used for
    identification of SSC (approx 1 SC in 15 total
    cells) using FACS or MACS

16
Markers of spermatogonial stem cells
  • Thy -1



  • ß-1 and a6 integrin
  • Stra 8
  • CD9 antigen
  • c-Kit receptor
  • Spermatogonial stem cells share some, but not all
    phenotypic and functional characteristics with
    other stem cells.


17
Self-renewal
  • Self-renewal maintains spermatogenesis
  • Factors regulating the self-renewal and
    differentiation
  • Intrinsic gene expression
  • Extrinsic signals (soluble factors)
  • Adhesion of molecules
  • Regulatory mechanism remains elusive

18
Spermatogonial control mechanism
  • Sertoli cells limits the expansion of SSC
    population
  • Hormones do not influence the expansion of
    spermatogonial cells
  • Regulated automatically or genetically
  • Stem Cell Factor and its receptor c-kit regulate
    spermatogonial development

19
Culture
  • SSCs maintained in culture without losing their
    proliferation and differentiation potential.

  • (Nagano et al., 1998)
  • SSCs maintained in co-culture with sertoli cells
    without loosing the ability to replicate their
    DNA.

  • (Van Der Wee et al., 2001)
  • SCF and GM-CSF enhance the survival of porcine
    type A SSCs (Dirami et al., 1999)
  • SSCs can expand in complete absence of serum or
    somatic feeder cells in vitro.

  • (Kanatsu-Shinohara et al., 2005)
  • SSCs can undergo anchorage-independent,
    self-renewal division in vitro.

  • (Kanatsu-Shinohara et al., 2006)

20
Cryopreservation of SSCs
  • Successful transplantation after freezing the
    donor tissue for 156 days
  • (Avarbock and colleagues, 1996 )
  • Frozen thawed bovine SSCs survive
    cryopreservation maintained during co-culture,
    maintenance is influenced by GDNF.
  • Donor testis cells isolated from different
    species frozen up to 96 days at 196 C were able
    to generate spermatogenesis in recipient
    seminiferous tubules.


    (Avarbock et al., 1996)
  • Cryopreserved testis cells of dogs and rabbits
    are capable of colonizing the recipient mouse
    testis.

  • (Dobrinski et al.,1999)
  • Bovine type A spermatogonia survived after 2-4
    months of cryopreservation.

  • (Izadyar et al.,2002)

21
Genes responsible for SSCs maintenance
  • Stage specific expression of Tsp57 mRNA
    indicates that it has very specific role during
    the haploid phase of spermatogenesis.

    (Kim et al., 2004)
  • Pin-1 is required to regulate proliferation and
    cell fate of undifferentiated spermatogonia in
    the adult mouse testis.
    (Atchison et al.,
    2003)
  • Plzf null mice share similar defects in sperm
    production that are due to an inability of
    spermatogonial stem cells to self renew.

    (Kotaja et al., 2004)
  • Dazl expression is predominant in the primary
    spermatocytes and weak in spermatogonia.

    (Lin et al., 2001)
  • Maintenance of spermatogenesis requires TAF4b and
    a requisite for fertility in mice.


    (Falender et al., 2005)
  • Bcl6b is a critical molecule for SSC function and
    also an important component in maintaining normal
    SSC biology and spermatogenesis in vivo.

22
Transplantation of SSCs
  • Brinster and Zimmerman in 1994- Ist time
  • Cellular differentiation was also started after
    injecting the cellular suspension
  • They found that donor- derived spermatogonia were
    responsible for producing offspring
  • Transplantation between greater distant animals
    has been less successful. This is likely due to
    failed spermatogonia and sertoli cell structural
    association and other functional interactions.
  • As a result
  • Production of morphologically defective
    spermatozoa
  • Successful spermatogenesis obtained following
    human-to-rat and mouse transplantation
    (Sofikitis et al, 1999)
  • Human to immunodeficient mouse testicular tissue
    transplantation, no evidence of donor tissue
    survival.
    ( Reis et al, 2000)

23
  • Human spermatogonia in mouse survived up to 6
    months but no meiotic activity was found in
    donor tissues (Nagano et al,
    2002)
  • Mouse seminiferous tubules provide a suitable
    environment for germ cells from distant species
    to interact with supporting cells and associate
    with basement membrane.

    (Dobrinski et al., 1999)
  • Transplantation of hamster germ cells into mouse
    testes resulted in donor-derived spermatogenesis.
    (Ogawa et al.,
    1999)
  • Successful transplantation of bovine type A
    spermatogonia in recipient bulls resulting in
    full spermatogenesis after autologus
    transplantation.
    (F.Izadyar et al., 2003)

24
  • To date, donorderived spermatogenesis has been
    primarily limited to similar species
  • Mouse-tomouse, Rat-to-mouse, Hamster-to-mouse
  • It has been said that evolutionary distance is
    primarily responsible for the failure of
    transplantation
  • Success was obtained in similar species only

25
  • Spermatogonial stem cells transplantation would
    act as a wonderful tool to
  • Study the early male germ cell development.
  • Study the surface markers.
  • Study the genes factors involved in regulation
    of proliferation and differentiation of
    spermatogonial stem cells.
  • Preservation of germ line in valuable males.
  • Transgenic animals.

26
Practical implications
  1. Spermatogenic process can be reinitiated in the
    patients those who have lost their spermatogonial
    cells during the treatment for such diseases.
  2. Transplantation of spermatogonial stem cells in
    the recipients seminiferous tubules for
    reinitiation of spermatozoa production in injury
    and other cytotoxic damages
  3. In-vitro spermatogenesis
  4. Production of transgenic animals (more easy than
    the ESC technique)
  5. Development of male contraception
  6. Cryopreservation of reserve sperms and combined
    with artificial reproduction techniques.
  7. Animal conservation
  8. Multipotent adult germline stem cells can be used
    for individual cell based therapy without the
    ethical and immunological problems associated
    with human embryonic stem cells
  9. Acts as precursor in case of natural depletion
  10. Alternative strategy for fertility preservation

27
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