| Literature DB >> 24826378 |
Vladislav Volarevic1, Sanja Bojic1, Jasmin Nurkovic1, Ana Volarevic1, Biljana Ljujic1, Nebojsa Arsenijevic1, Majlinda Lako2, Miodrag Stojkovic3.
Abstract
Stem cells are undifferentiated cells that are present in the embryonic, fetal, and adult stages of life and give rise to differentiated cells that make up the building blocks of tissue and organs. Due to their unlimited source and high differentiation potential, stem cells are considered as potentially new therapeutic agents for the treatment of infertility. Stem cells could be stimulated in vitro to develop various numbers of specialized cells including male and female gametes suggesting their potential use in reproductive medicine. During past few years a considerable progress in the derivation of male germ cells from pluripotent stem cells has been made. In addition, stem cell-based strategies for ovarian regeneration and oocyte production have been proposed as future clinical therapies for treating infertility in women. In this review, we summarized current knowledge and present future perspectives and challenges regarding the use of stem cells in reproductive medicine.Entities:
Mesh:
Year: 2014 PMID: 24826378 PMCID: PMC4009115 DOI: 10.1155/2014/507234
Source DB: PubMed Journal: Biomed Res Int Impact factor: 3.411
Characteristics of stem cells used in stem cell-based therapy of infertility.
| ESCs | MSCs | Stem cell from extraembryonic tissues | iPSCs | Spermatogonial stem cells |
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| Derived from inner cell mass of the blastocyst | Derived from bone marrow, adipose tissues, bone, Wharton's jelly, umbilical cord blood, and peripheral blood | Derived from amnion, chorion, placenta, and umbilical cord | Derived from somatic cells | Derived from testicular tissues |
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| Pluripotent | Multipotent | Multipotent | Pluripotent | Pluripotent |
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| These cells can differentiate into cell types of all three germ layers | These cells can differentiate into mesoderm-derived tissues (adipose tissues, bon, cartilage, and muscle) | These cells can differentiate into adipocytes, endothelial cells, hepatocytes, osteocytes, myocytes, and neurons | These cells can differentiate into cell types of all three germ layers | These cells can differentiate into cell types of all three germ layers |
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| Prolonged proliferation | Degree of proliferation depends on the tissue from which these cells were isolated | Degree of proliferation depends on the tissue from which these cells were isolated | Prolonged proliferation | Difficult to be maintained in cultures |
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| Indefinite self-renewal potential | Limited self-renewal | Limited self-renewal | Indefinite self-renewal potential | Self-renewal ability to go through numerous cell divisions while maintaining the undifferentiated state |
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| High telomerase activity | Low telomerase activity | Low telomerase activity | High telomerase activity | High telomerase activity |
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| Immortal; cell lines remain intact for long periods of time and produce endless numbers of cells | Production of limited number of cells | Production of limited number of cells | Immortal; cell lines remain intact for long periods of time and produce endless numbers of cells | — |
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| These cells are not immune privileged | These cells have immunomodulatory characteristics | — | These cells are not immune privileged | These cells are not immune privileged |
Potential advantages and disadvantages of stem cells in regenerative medicine.
| Stem cells | Advantages | Disadvantages |
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| ESCs | Pluripotent; high telomerase activity | Ethical concerns; malignant potential; difficult to control; may require many steps to differentiate into desired cell type; immune rejection |
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| MSCs | No ethical or moral concerns; low malignant potential; avoiding allogeneic immune rejection | Limited flexibility; multipotent; difficulty to be maintained in cell culture for long periods |
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| Stem cell from extraembryonic tissues | No ethical or moral concerns; reducing risk of tumorigenicity | Limited flexibility; multipotent |
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| iPSCs | No ethical or moral concerns; patient-specific cells | Use of viral vectors to introduce genes; malignant potential |
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| Spermatogonial stem cells | No ethical or moral concerns | Relatively small numbers in testis; difficulty to be maintained in cultures; immune rejection |
Figure 1Stem cell-derived male gametes. Several growth factors and cytokines are used for in vitro differentiation of pluripotent cells into male gametes/SSC-like cells. The transplantation of stem cell-derived SSC-like cells in sterile mice results in proper spermatogenesis.
Figure 2Ovarian stem cells:isolation and regenerative potential. Ovarian stem cells (MVH+BrdU+ cells) residing within the ovarian surface epithelium of neonatal and adult mice express high telomerase activity, Oct4, and Nanog and have a capacity to generate functional oocytes when transplanted back into sterile recipient mice.