New oncolytic virus platform to treat cancers with myxoma virus

What is claimed is: 1 . A myxoma virus (MYXV) having enhanced anti-cancer activity, wherein the MYXV is genetically engineered to attenuate an activity or expression level of its M153 protein. 2 . The MYXV of claim 1 , wherein the activity or the expression level of the M153 protein is attenuated at least 80%. 3 . The MYXV of claim 1 , wherein the MYXV is engineered to introduce a mutation in a nucleic acid encoding the M153 protein, wherein the mutation comprises an insertion, deletion, or substitution mutation. 4 . The MYXV of claim 1 , wherein at least a portion of a nucleic acid encoding the M153 protein in MYXV genome is knocked out. 5 . The MYXV of claim 1 , wherein the MYXV comprises an inhibitory molecule targeting M153 transcript that thereby attenuates the M153 protein expression, wherein the inhibitory molecule comprises dsRNA, siRNA, antisense RNA, or miRNA. 6 . The MYXV of claim 1 , wherein the MYXV is further genetically engineered to express a non-viral molecule. 7 . The MYXV of claim 6 , wherein the non-viral molecule is a cytokine or a cell matrix protein. 8 . The MYXV of claim 7 , wherein the non-viral molecule is tumor necrosis factor alpha (TNFα), interleukin-12 subunit alpha (IL-12α), interleukin-12 subunit beta (IL-12β), or decorin. 9 . The MYXV of claim 6 , wherein the non-viral molecule is a human protein. 10 . The MYXV of claim 1 , wherein the MYXV expresses at least two non-viral molecules selected from a group consisting of TNFα, IL-12α, IL-12β, and decorin. 11 . A composition comprising a plurality of cells treated ex vivo by a MYXV, wherein the MYXV is genetically engineered to attenuate an activity or expression level of its M153 protein, and to express a non-viral molecule. 12 . The composition of claim 11 , wherein the plurality of cells comprises peripheral blood mononuclear cells (PBMCs), bone marrow (BM) cells, or a combination thereof. 13 . A recombinant nucleic acid comprising at least a portion of MYXV genome, wherein the portion of the MYXV genome is modified to reduce expression of M153 gene. 14 . The recombinant nucleic acid of claim 13 , wherein the portion of MYXV genome is modified to knock out at least a portion of the M153 gene in the portion of MYXV genome. 15 . The recombinant nucleic acid of claim 13 , comprising a nucleic acid encoding a non-viral molecule. 16 . The recombinant nucleic acid of claim 15 , wherein the non-viral molecule is human TNFα, human IL-12α (hTNFα), human IL-12β, or human decorin. 17 . The recombinant nucleic acid of claim 15 , wherein the nucleic acid encoding the non-viral molecule comprises a vMyx-hTNFα cassette, and the nucleic acid encoding the non-viral molecule replaces or is adjacent to an M135R gene of the MYXV genome. 18 . The recombinant nucleic acid of claim 15 , wherein the nucleic acid encoding the non-viral molecule comprises a vMyx-hTNFα cassette, and the nucleic acid encoding the non-viral molecule is inserted between an M135R gene and an M136R gene of the MYXV genome. 19 . The recombinant nucleic acid of claim 15 , wherein the nucleic acid encoding the non-viral molecule comprises an hDecorin-hIL-12 cassette, and the nucleic acid encoding the non-viral molecule replaces at least a portion of the M153 gene of the MYXV genome. 20 . The recombinant nucleic acid of claim 15 , wherein the nucleic acid encoding the non-viral molecule comprises a vMyx-hTNFα-hDecorin-hIL-12-M153KO (vMyx-Triple) cassette. 21 . A method of inhibiting, alleviating, or preventing a cancer in a subject in need thereof, comprising administering to the subject a MYXV or a plurality of cells treated with the MYXV, wherein the MYXV is genetically engineered to attenuate an activity or expression level of its M153 protein. 22 . The method of claim 21 , wherein the MYXV is further genetically engineered to express a non-viral molecule. 23 . The method of claim 22 , wherein the non-viral molecule is tumor necrosis factor alpha (TNFα), interleukin-12 subunit alpha (IL-12α), interleukin-12 subunit beta (IL-12β), or decorin. 24 . The method of claim 21 , wherein the MYXV or the plurality of cells is administered by systemic administration. 25 . The method of claim 21 , wherein the administration reduces tumor cell viability, or activates immunogenic cell death in the cancer. 26 . The method of claim 21 , wherein the cancer is a solid tumor, an osteosarcoma, triple negative breast cancer, or melanoma. 27 . The method of claim 21 , wherein the cancer has metastasized to a lung, a brain, a liver or a lymph node in the subject. 28 . The method of claim 21 , further comprising administering to the subject an immune checkpoint modulator. 29 . The method of claim 21 , wherein the administration is performed in a dose and a schedule effective to increase expression of at least two cytokines in PBMC or cancer cells of the subject, wherein the at least two cytokines comprise IFN-γ, IL-2, IL-6, IL-10, IL-12, or TNF-α. 30 . The method of claim 21 , wherein the administration is performed in a dose and a schedule effective to reduce volume of the cancer at least 10%.