Hepatocellular carcinoma (HCC) is one of the most common cancers in the world, particularly in Asia and Africa. Due to its highly neovascularization, anti-angiogenic approach could be a potential therapeutic strategy. Ultrasound (US) is an effective tool to locally deliver genes into target tumors or organs. US, in combination with microbubbles SonoVue®, can temporarily change the permeability of cell membranes by cavitation and thus enhances the delivery of plasmid DNA into cells. In the first part of this study, we compared the efficiency of US-mediated gene delivery at different sites, i.e., the orthotopic liver tumor, the subcutaneous tumor or the muscle. We injected luciferase, IL-12 or EGFP plasmid DNA mixed with SonoVue® into BALB/c mice either intramuscularly (IM) or intratumorally (IT), followed by exposure to US. We found that intramuscular injection provided better expression results than intratumoral injection. In the second part of this research, we assessed the therapeutic effects of US-mediated IM gene therapy on three previously established liver tumor models, namely subcutaneous tumor model, implanted liver tumor model and primary multifocal HCC model. We delivered the endostatin (ED) or the calreticulin (CRT) gene, both of which are anti-angiogenic factors through IM injection. The experimental results showed that four times of IM ultrasound treatment yielded significant therapeutic effects on these three liver tumor models and also prolonged the survival time in mice. Furthermore, immunohistochemical staining of the tumors revealed increased tumor-infiltrating T lymphocytes and apoptotic cells which were probably induced by the decreased neovascularization. We also combined immunotherapy with anti-angiogenic therapy, using recombinant adenoviruses carrying GM-CSF and IL-12 genes followed by ultrasound delivery of ED or CRT gene. The combined therapy showed much better therapeutic effects on both implanted and primary multifocal HCC models than either therapy alone. In this combined therapy, a very significant increase in tumor-infiltrating T cells and a further decrease in tumor vascularization were observed. In addition, combination of chemotherapy using doxorubicin with anti-angiogenic therapy also provided a better therapeutic effect than either therapy alone. Taken together, we have proved for the first time that co-injection of microbubbles and plasmid DNA intramuscularly followed by ultrasound exposure can effectively provide a cure for liver cancers, and this strategy may have therapeutic potential for the clinical treatment.