Composition of mesenchymal stem cells

We claim: 1 . A method of preparing a composition suitable for a mesenchymal stem cell (MSC) treatment of a mammal, wherein the preparation method comprises: a. obtaining a gingival tissue, b. separating the gingival tissue into cells, c. sorting neural crest derived gingiva mesenchymal stem cells (N-GMSCs), and d. preparing a composition comprising N-GMSCs. 2 . The preparation method of claim 1 , wherein the mammal is a human. 3 . The preparation method of claim 1 , wherein the mammal is a non-human animal. 4 . The preparation method of claim 1 , wherein separating the gingival tissue into cells is done by a mechanical method, a chemical method, or a combination of a mechanical and a chemical method. 5 . The preparation method of claim 4 , wherein the chemical method is an enzymatic digestion method. 6 . The preparation method of claim 5 , wherein the enzymatic digestion method comprises digesting the gingival tissue by using a solution comprising a collagenase and a dispase, and thereby obtaining a digested gingival tissue. 7 . The preparation method of claim 6 , wherein the collagenase is collagenase type I and the dispase is dispase II. 8 . The preparation method of claim 6 , wherein separating the gingival tissue into cells comprises preparing cell suspensions from the digested gingival tissue using a mechanical method. 9 . The preparation method of claim 8 , wherein the mechanical method comprises filtering the digested gingival tissue to obtain cell suspensions. 10 . The preparation method of claim 9 , wherein the cell suspensions are single-cell suspensions. 11 . The preparation method of claim 8 , wherein the preparation method further comprises culturing the separated cells before sorting N-GMSCs. 12 . The preparation method of claim 11 , wherein culturing the separated cells comprises providing a solid surface, seeding the cells on the solid surface, culturing the seeded cells, and thereby obtaining a culture comprising cells that are adherent to the solid surface and cells that are not adherent to the solid surface. 13 . The preparation method of claim 12 , wherein the method further comprises eliminating from the culture the cells that are not adherent to the solid surface. 14 . The preparation method of claim 13 , wherein the method further comprises dissociating from the solid surface the cells that are adherent to the solid surface. 15 . The preparation method of claim 14 , wherein the method further comprises dissociating from the solid surface by using an enzyme those cells that are adherent to the solid surface. 16 . The preparation method of claim 14 , wherein the method further comprises dissociating from the solid surface by using trypsin those cells that are adherent to the solid surface. 17 . The preparation method of claim 12 , wherein the method further comprises expanding the cultured cells. 18 . The preparation method of claim 1 , wherein the sorting comprises sorting fluorescein isothiocyanate positive cells as N-GMSCs. 19 . The preparation method of claim 11 , wherein the sorting comprises sorting fluorescein isothiocyanate positive cells as N-GMSCs. 20 . A method of treating a mammal using a composition comprising N-GMSCs. 21 . The treatment method of claim 20 , wherein treating the mammal comprises using the composition to regenerate neural tissue. 22 . The treatment method of claim 20 , wherein treating the mammal comprises using the composition to repair damaged cartilage. 23 . The treatment method of claim 20 , wherein treating the mammal comprises using the composition to induce activated T cell apoptosis. 24 . The treatment method of claim 20 , wherein treating the mammal comprises using the composition to heal a wound and/or to treat inflammatory diseases and/or autoimmune diseases. 25 . The treatment method of claim 20 , wherein treating the mammal comprises using the composition to treat graft-versus-host disease (GvHD), diabetes, rheumatoid arthritis (RA), autoimmune encephalomyelitis, systemic lupus erythematosus (SLE), multiple sclerosis (MS), periodontitis, inflammatory bowel disease (IBD), alimentary tract mucositis induced by chemo- or radiotherapy, and sepsis. 26 . The treatment method of claim 20 , wherein treating the mammal comprises using the composition to reduce wrinkles, and/or for soft tissue augmentation and/or skin rejuvenation. 27 . The treatment method of claim 20 , wherein treating the mammal comprises using the composition to suppress peripheral blood lymphocyte proliferation or to induce the expression of immunosuppressive factors. 28 . The treatment method of claim 20 , wherein treating the mammal comprises using the composition to induce the expression of interleukin 10 (IL-10), indoleamine 2,3-dioxygenase (IDO), nitric oxide synthase (iNOS), and cyclooxygenase-2 (COX-2). 29 . The treatment method of claim 20 , wherein the mammal is a human. 30 . The treatment method of claim 20 , wherein the mammal is a non-human.