Journal of Plant Biotechnology

  • 제33권3호
  • /
  • Pages.195-207
  • /
  • 2006
  • /
  • 1229-2818(pISSN)
  • /
  • 2384-1397(eISSN)
한국식물생명공학회 (The Korean Society of Plant Biotechnology)
권호 표지
DOI QR코드

DOI QR Code

Stem Cell Biology, 최근의 진보

Recent Advancement in the Stem Cell Biology

  • 발행 : 2006.09.30
PDF 다운로드
⟨ 이전 논문 다음 논문 ⟩

초록

Stem cells are the primordial, initial cells which usually divide asymmetrically giving rise to on the one hand self-renewals and on the other hand progenitor cells with potential for differentiation. Zygote (fertilized egg), with totipotency, deserves the top-ranking stem cell - he totipotent stem cell (TSC). Both the ICM (inner cell mass) taken from the 6 days-old human blastocyst and ESC (embryonic stem cell) derived from the in vitro cultured ICM have slightly less potency for differentiation than the zygote, and are termed pluripotent stem cells. Stem cells in the tissues and organs of fetus, infant, and adult have highly reduced potency and committed to produce only progenitor cells for particular tissues. These tissue-specific stem cells are called multipotent stem cells. These tissue-specific/committed multipotent stem cells, when placed in altered environment other than their original niche, can yield cells characteristic of the altered environment. These findings are certainly of potential interest from the clinical, therapeutic perspective. The controversial terminology 'somatic stem cell plasticity' coined by the stem cell community seems to have been proved true. Followings are some of the recent knowledges related to the stem cell. Just as the tissues of our body have their own multipotent stem cells, cancerous tumor has undifferentiated cells known as cancer stem cell (CSC). Each time CSC cleaves, it makes two daughter cells with different fate. One is endowed with immortality, the remarkable ability to divide indefinitely, while the other progeny cell divides occasionally but lives forever. In the cancer tumor, CSC is minority being as few as 3-5% of the tumor mass but it is the culprit behind the tumor-malignancy, metastasis, and recurrence of cancer. CSC is like a master print. As long as the original exists, copies can be made and the disease can persist. If the CSC is destroyed, cancer tumor can't grow. In the decades-long cancer therapy, efforts were focused on the reducing of the bulk of cancerous growth. How cancer therapy is changing to destroy the origin of tumor, the CSC. The next generation of treatments should be to recognize and target the root cause of cancerous growth, the CSC, rather than the reducing of the bulk of tumor, Now the strategy is to find a way to identify and isolate the stem cells. The surfaces of normal as well as the cancer stem cells are studded with proteins. In leukaemia stem cell, for example, protein CD 34 is identified. In the new treatment of cancer disease it is needed to look for protein unique to the CSC. Blocking the stem cell's source of nutrients might be another effective strategy. The mystery of sternness of stem cells has begun to be deciphered. ESC can replicate indefinitely and yet retains the potential to turn into any kind of differentiated cells. Polycomb group protein such as Suz 12 repress most of the regulatory genes which, activated, are turned to be developmental genes. These protein molecules keep the ESC in an undifferentiated state. Many of the regulator genes silenced by polycomb proteins are also occupied by such ESC transcription factors as Oct 4, Sox 2, and Nanog. Both polycomb and transcription factor proteins seem to cooperate to keep the ESC in an undifferentiated state, pluripotent, and self-renewable. A normal prion protein (PrP) is found throughout the body from blood to the brain. Prion diseases such as mad cow disease (bovine spongiform encephalopathy) are caused when a normal prion protein misfolds to give rise to PrP$^{SC}$ and assault brain tissue. Why has human body kept such a deadly and enigmatic protein? Although our body has preserved the prion protein, prion diseases are of rare occurrence. Deadly prion diseases have been intensively studied, but normal prion problems are not. Very few facts on the benefit of prion proteins have been known so far. It was found that PrP was hugely expressed on the stem cell surface of bone marrow and on the cells of neural progenitor, PrP seems to have some function in cell maturation and facilitate the division of stem cells and their self-renewal. PrP also might help guide the decision of neural progenitor cell to become a neuron.

키워드

참고문헌

  1. AI-Hajj M, Clarke MF (2004) Self-renewal and solid tumor stem cells. Oncogene 23: 7274-7282 https://doi.org/10.1038/sj.onc.1207947
  2. Bell DR, Zant GV (2004) Stem cells, aging, and cancer : inevitabilities and outcomes. Oncogene 23:. 7290-7296 https://doi.org/10.1038/sj.onc.1207949
  3. Blackburn E (2001) Switching and signaling at the telomere. Cell 106: 661-673 https://doi.org/10.1016/S0092-8674(01)00492-5
  4. Blanpain C, Lowry WE, Geoghegan A, Polak L, Fuchs E (2004) Self-renewal, multipotency, and the existence of two cell populations within an epithelial stem cell niche. Cell 118: 635-648 https://doi.org/10.1016/j.cell.2004.08.012
  5. Braun KM, Niemann C, Jensen UB, Sundberg JP, SilvaVargas V, Watt FM (2003) Manipulation of stem cell proliferation and lineage commitment: visualization of label-retaining cells in wholemounts of mouse epidermis. Development 130: 5241-5255 https://doi.org/10.1242/dev.00703
  6. Couzin J (2006) The prion protein has a good side? You bet. Science 311: 1091 https://doi.org/10.1126/science.311.5764.1091
  7. Flores I, Cayuela ML, Blasco MA (2005) Effects of telomerase and telomere length on epidermal stem cell behavior. Science 309: 1253-1256 https://doi.org/10.1126/science.1115025
  8. Gage FH (2000) Mammalian neural stem cells. Science 287: 1433-1438 https://doi.org/10.1126/science.287.5457.1433
  9. Giri RK, Young R, Pitstick R, DeArmond SJ, Prusiner SB, Carlson G (2006) Prion infection of mouse neurospheres. Proc Natl Acad Sci 103: 3875-3880
  10. Golding MC, Long CR, Carmell MA, Hannon GJ, Westhusin M (2006) Suppression of prion protein in livestock by RNA interference. Proc Natl Acad Sci 103: 5285-5290
  11. Ham C (2000) Mammalian cloning by nuclear transfer, stem cell, and enzyme telomerase. Korean J Plant Tissue Culture 27: 423-428
  12. Harrington L (2004) Does the reservoir for self-renewal stem from the ends? Oncogene 23: 7283-7285 https://doi.org/10.1038/sj.onc.1207948
  13. Holden C (2006) Gene-suppressing proteins reveal secrets of stem cells. Science 312: 349
  14. Lange TD (2001) Telomere capping - One strand fits all. Science 293: 1075-1076
  15. Shay JW, Wright WE (2005) Senescence and immortalization: role of telomeres and telomerase. Carcinogenesis 26: 867-874 https://doi.org/10.1093/carcin/bgh296
  16. Singh MB, Bhalla PL (2006) Plant stem cells carve their own niche. Trends in Plant Sci 11: 241-246 https://doi.org/10.1016/j.tplants.2006.03.004
  17. Steele AD, Emsley JG, Ozdinler PH, Lindquist S, Macklis JD (2006) Prion protein (PrPC) positively regulates neural precursor proliferation during developmental and adult mammalian neurogenesis. Proc Natl Acad Sci 103: 3416-3421
  18. Tumber T, Guasch G, Greco V, Blanpain C, Lowry WE, Rendl M, Fuchs E (2004) Defining the epitherial stem cell niche in skin. Science 303: 359-363 https://doi.org/10.1126/science.1092436
  19. Watt FM, Hogan BLM (2000) Out of Eden: stem cells and their niches. Science 287: 1427-1430 https://doi.org/10.1126/science.287.5457.1427
  20. Zant GV, Liang Y (2003) The role of stem cells in aging. Experimental Hematology 31: 659-672 https://doi.org/10.1016/S0301-472X(03)00088-2
  21. Zhang CC, Steele AD, Lindquist S, Lodish HF (2006) Prion protein is expressed on long-term repopulating hematopoietic stem cells and is important for their self-renewal. Proc Natl Acad Sci 103: 2184-2189