Progress on the Plasticity of Muscle-derived Stem Cell

China Biotechnology

2011, Vol. 31

Issue (7): 114-120 DOI:

Progress on the Plasticity of Muscle-derived Stem Cell

WU Xiao-yun, WANG Shi-li

Key Laboratory of Biotech-Drugs, Ministry of Health, Shandong Medicinal Biotechnology Center, Jinan 250062, China

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Abstract

Two types of stem cells in muscle: satellite cells and muscle-derived stem cells (MDSCs) have been identified. MDSCs, a predecessor of the satellite cell, are considered to possess a higher regeneration capacity and to exhibit better cell survival and a broader range of multilineage capabilities. MDSCs are not only able to differentiate into mesodermal cell types including the myogenic, adipogenic, osteogenic, chondrogenic, endothelial, and hematopoietic lineages, but also possess the potential to break germ layer commitment and differentiate into ectodermal and endodermal lineages under certain conditions. The progress on isolation, identification, plasticity, and the current clinical applications of MDSCs are reviewed.

Key words： Muscle-derived stem cells Plasticity Isolation Differentiation Gene therapy Tissue regeneration

Received: 21 September 2010 Published: 25 July 2011

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WU Xiao-yun, WANG Shi-li. Progress on the Plasticity of Muscle-derived Stem Cell. China Biotechnology, 2011, 31(7): 114-120.

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https://manu60.magtech.com.cn/biotech/ OR https://manu60.magtech.com.cn/biotech/Y2011/V31/I7/114

[1] Wu X, Wang S, Chen B, et al. Muscle-derived stem cells: isolation, characterization, differentiation, and application in cell and gene therapy. Cell Tissue Res, 2010, 340(3):549-567.

[2] Vourch P, Romero-Ramos M, Chivatakarn O, et al. Isolation and characterization of cells with neurogenic potential from adult skeletal muscle. Biochem Biophys Res Commun, 2004, 317(3):893-901.

[3] Arsic N, Mamaeva D, Lamb N J, et al. Muscle-derived stem cells isolated as non-adherent population give rise to cardiac, skeletal muscle and neural lineages. Exp Cell Res, 2008, 314(6):1266-1280.

[4] Gharaibeh B, Lu A, Tebbets J, et al. Isolation of a slowly adhering cell fraction containing stem cells from murine skeletal muscle by the preplate technique. Nat Protoc, 2008, 3(9):1501-1509.

[5] Wei Y, Li Y, Chen C, et al. Human skeletal muscle-derived stem cells retain stem cell properties after expansion in myosphere culture. Exp Cell Res, 2011, 317(7):1016-1027.

[6] Sherwood R I, Christensen J L, Conboy I M, et al. Isolation of adult mouse myogenic progenitors: functional heterogeneity of cells within and engrafting skeletal muscle. Cell, 2004, 119(4):543-554.

[7] Bauermeister K T, Stolting S, Kaczmarek P M, et al. Hematopoietic progenitor cells residing in muscle engraft into bone marrow following transplantation. Int J Hematol, 2004, 79(5):488-494.

[8] Tsuboi K, Kawada H, Toh E, et al. Potential and origin of the hematopoietic population in human skeletal muscle. Leuk Res, 2005, 29(3):317-324.

[9] McKinney-Freeman S L, Jackson K A, Camargo F D, et al. Muscle-derived hematopoietic stem cells are hematopoietic in origin. Proc Natl Acad Sci U S A, 2002, 99(3):1341-1346.

[10] Jiang Y, Vaessen B, Lenvik T, et al. Multipotent progenitor cells can be isolated from postnatal murine bone marrow, muscle, and brain. Exp Hematol, 2002, 30(8):896-904.

[11] Jiang Y, Jahagirdar B N, Reinhardt R L, et al. Pluripotency of mesenchymal stem cells derived from adult marrow. Nature, 2002, 418(6893):41-49.

[12] Ji K H, Xiong J, Hu K M, et al. Simultaneous expression of Oct4 and genes of three germ layers in single cell-derived multipotent adult progenitor cells. Ann Hematol, 2008, 87(6):431-438.

[13] Aranguren X L, Luttun A, Clavel C, et al. In vitro and in vivo arterial differentiation of human multipotent adult progenitor cells. Blood, 2007, 109(6):2634-2642.

[14] Zhong J F, Zhan Y, Anderson W F, et al. Murine hematopoietic stem cell distribution and proliferation in ablated and nonablated bone marrow transplantation. Blood, 2002, 100(10):3521-3526.

[15] Negroni E, Riederer I, Chaouch S, et al. In vivo myogenic potential of human CD133(+) muscle-derived stem cells: a quantitative study. Mol Ther, 2009.

[16] Tamaki T, Akatsuka A, Ando K, et al. Identification of myogenic-endothelial progenitor cells in the interstitial spaces of skeletal muscle. J Cell Biol, 2002, 157(4):571-577.

[17] Tamaki T, Uchiyama Y, Okada Y, et al. Functional recovery of damaged skeletal muscle through synchronized vasculogenesis, myogenesis, and neurogenesis by muscle-derived stem cells. Circulation, 2005, 112(18):2857-2866.

[18] Tamaki T, Okada Y, Uchiyama Y, et al. Synchronized reconstitution of muscle fibers, peripheral nerves and blood vessels by murine skeletal muscle-derived CD34(-)/45 (-) cells. Histochem Cell Biol, 2007, 128(4):349-360.

[19] Sacco A, Doyonnas R, Kraft P, et al. Self-renewal and expansion of single transplanted muscle stem cells. Nature, 2008, 456(7221):502-506.

[20] Seaberg R M, Smukler S R, Kieffer T J, et al. Clonal identification of multipotent precursors from adult mouse pancreas that generate neural and pancreatic lineages. Nat Biotechnol, 2004, 22(9):1115-1124.

[21] Tamaki T, Okada Y, Uchiyama Y, et al. Clonal multipotency of skeletal muscle-derived stem cells between mesodermal and ectodermal lineage. Stem Cells, 2007, 25(9):2283-2290.

[22] Tamaki T, Okada Y, Uchiyama Y, et al. Skeletal muscle-derived CD34+/45-and CD34-/45-stem cells are situated hierarchically upstream of Pax7+ cells. Stem Cells Dev, 2008, 17(4):653-667.

[23] Tamaki T, Akatsuka A, Okada Y, et al. Cardiomyocyte formation by skeletal muscle-derived multi-myogenic stem cells after transplantation into infarcted myocardium. PLoS One, 2008, 3(3):e1789.

[24] Tamaki T, Uchiyama Y, Okada Y, et al. Clonal Differentiation of Skeletal Muscle-Derived CD34-/45-Stem Cells into Cardiomyocytes in vivo. Stem Cells Dev, 2009.

[25] Zheng B, Cao B, Crisan M, et al. Prospective identification of myogenic endothelial cells in human skeletal muscle. Nat Biotechnol, 2007, 25(9):1025-1034.

[26] Gerald A. The heterogeneity of clonally derived purified murine marrow stem cell colonies. Blood, 2005.

[27] Wright V, Peng H, Usas A, et al. BMP4-expressing muscle-derived stem cells differentiate into osteogenic lineage and improve bone healing in immunocompetent mice. Mol Ther, 2002, 6(2):169-178.

[28] Usas A, Ho A M, Cooper G M, et al. Bone regeneration mediated by BMP4-expressing muscle-derived stem cells is affected by delivery system. Tissue Eng Part A, 2009, 15(2):285-293.

[29] Shen H C, Peng H, Usas A, et al. Ex vivo gene therapy-induced endochondral bone formation: comparison of muscle-derived stem cells and different subpopulations of primary muscle-derived cells. Bone, 2004, 34(6):982-992.

[30] Adachi N, Sato K, Usas A, et al. Muscle derived, cell based ex vivo gene therapy for treatment of full thickness articular cartilage defects. J Rheumatol, 2002, 29(9):1920-1930.

[31] Goldring M B. Are bone morphogenetic proteins effective inducers of cartilage repair? Ex vivo transduction of muscle-derived stem cells. Arthritis Rheum, 2006, 54(2):387-389.

[32] Payne T R, Oshima H, Sakai T, et al. Regeneration of dystrophin-expressing myocytes in the mdx heart by skeletal muscle stem cells. Gene Ther, 2005, 12(16):1264-1274.

[33] Ikezawa M, Cao B, Qu Z, et al. Dystrophin delivery in dystrophin-deficient DMDmdx skeletal muscle by isogenic muscle-derived stem cell transplantation. Hum Gene Ther, 2003, 14(16):1535-1546.

[34] Baek Y S, Kang S H, Park J S, et al. Long-term cultured skeletal muscle-derived neural precursor cells and their neurogenic potentials. Neuroreport, 2009, 20(12):1109-1114.

[35] Schultz S S, Lucas P A. Human stem cells isolated from adult skeletal muscle differentiate into neural phenotypes. J Neurosci Methods, 2006, 152(1-2):144-155.

[36] Allan D S, Jay K E, Bhatia M. Hematopoietic capacity of adult human skeletal muscle is negligible. Bone Marrow Transplant, 2005, 35(7):663-666.

[37] Farace F, Prestoz L, Badaoui S, et al. Evaluation of hematopoietic potential generated by transplantation of muscle-derived stem cells in mice. Stem Cells Dev, 2004, 13(1):83-92.

[38] Bueno D F, Kerkis I, Costa A M, et al. New source of muscle-derived stem cells with potential for alveolar bone reconstruction in cleft lip and/or palate patients. Tissue Eng Part A, 2009, 15(2):427-435.

[39] Kim K S, Lee J H, Ahn H H, et al. The osteogenic differentiation of rat muscle-derived stem cells in vivo within in situ-forming chitosan scaffolds. Biomaterials, 2008, 29(33):4420-4428.

[40] Corsi K A, Pollett J B, Phillippi J A, et al. Osteogenic potential of postnatal skeletal muscle-derived stem cells is influenced by donor sex. J Bone Miner Res, 2007, 22(10):1592-1602.

[41] Kubo S, Cooper G M, Matsumoto T, et al. Blocking vascular endothelial growth factor with soluble Flt-1 improves the chondrogenic potential of mouse skeletal muscle-derived stem cells. Arthritis Rheum, 2009, 60(1):155-165.

[42] Matsumoto T, Cooper G M, Gharaibeh B, et al. Cartilage repair in a rat model of osteoarthritis through intraarticular transplantation of muscle-derived stem cells expressing bone morphogenetic protein 4 and soluble Flt-1. Arthritis Rheum, 2009, 60(5):1390-1405.

[43] Claros S, Alonso M, Becerra J, et al. Selection and induction of rat skeletal muscle-derived cells to the chondro-osteogenic lineage. Cell Mol Biol (Noisy-le-grand), 2008, 54(1):1-10.

[44] Kondo T, Case J, Srour E F, et al. Skeletal muscle-derived progenitor cells exhibit neural competence. Neuroreport, 2006, 17(1):1-4.

[45] Arriero M, Brodsky S V, Gealekman O, et al. Adult skeletal muscle stem cells differentiate into endothelial lineage and ameliorate renal dysfunction after acute ischemia. Am J Physiol Renal Physiol, 2004, 287(4):F621-627.

[46] Nieponice A, Soletti L, Guan J, et al. Development of a tissue-engineered vascular graft combining a biodegradable scaffold, muscle-derived stem cells and a rotational vacuum seeding technique. Biomaterials, 2008, 29(7):825-833.

[47] Zhou C, Zhang C. Cell therapy for Duchenne muscular dystrophy. Zhonghua Yi Xue Yi Chuan Xue Za Zhi, 2006, 23(6):659-661.

[48] Chaouch S, Mouly V, Goyenvalle A, et al. Immortalized skin fibroblasts expressing conditional MyoD as a renewable and reliable source of converted human muscle cells to assess therapeutic strategies for muscular dystrophies: validation of an exon-skipping approach to restore dystrophin in duchenne muscular dystrophy cells. Hum Gene Ther, 2009, 20(7):784-790.

[49] Smaldone M C, Chancellor M B. Muscle derived stem cell therapy for stress urinary incontinence. World J Urol, 2008, 26(4):327-332.

[50] Kwon D, Kim Y, Pruchnic R, et al. Periurethral cellular injection: comparison of muscle-derived progenitor cells and fibroblasts with regard to efficacy and tissue contractility in an animal model of stress urinary incontinence. Urology, 2006, 68(2):449-454.

[51] Furuta A, Jankowski R J, Pruchnic R, et al. The potential of muscle-derived stem cells for stress urinary incontinence. Expert Opin Biol Ther, 2007, 7(10):1483-1486.

[52] Smaldone M C, Chen M L, Chancellor M B. Stem cell therapy for urethral sphincter regeneration. Minerva Urol Nefrol, 2009, 61(1):27-40.

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