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Human biofield therapy does not affect tumor size but modulates immune responses in a mouse model for breast cancer

Human biofield therapy does not affect tumor size but modulates immune responses in a mouse model for breast cancer

作     者:Gloria Gronowicz Eric R.Secor Jr. John R.Flynn Liisa T.Kuhn 

作者机构:Department of SurgeryUniversity of Connecticut Health Center Department of ImmunologyUniversity of Connecticut Health Center Hartford HealthcareHartford Hospital Department of Reconstructive SciencesUniversity of Connecticut Health Center 

出 版 物:《Journal of Integrative Medicine》 (结合医学学报(英文版))

年 卷 期:2016年第14卷第5期

页      面:389-399页

核心收录:

学科分类:1002[医学-临床医学] 100214[医学-肿瘤学] 10[医学] 

基  金:the Trivedi Foundation for funding this research 

主  题:biological therapy breast cancer immune system integrative medicine cytokine energymedicine 

摘      要:OBJECTIVE: To assess the effect of human biofield therapy, an integrative medicine modality, on the development of tumors and metastasis, and immune function in a mouse breast cancer model. METHODS: Mice were injected with 66cl4 mammary carcinoma cells. In study one, mice received biofield therapy after cell injection. In study two, mice were treated by the biofield practitioner only prior to cell injection. Both studies had two control groups of mock biofield treatments and phosphate- buffered saline injection. Mice were weighed and tumor volume was determined. Blood samples were collected and 32 serum cytokine/chemokine markers were measured. Spleens/popliteal lymph nodes were isolated and dissociated for fluorescent-activated cell sorting (FACS) analysis of immune cells or metastasis assays in cell culture. RESULTS: No signifcant differences were found in weight, tumor size or metastasis. Significant effects were found in the immune responses in study one but no additional effects were found in study two. In study one, human biofield treatment significantly reduced percentage of CD4~CD441oCD25~ and percentage of CD8~ cells, elevated by cancer in the lymph nodes, to control levels determined by FACS analysis. In the spleen, only CD11b~ macrophages were increased with cancer, and human biofield therapy significantly reduced them. Of 11 cytokines elevated by cancer, only interferon-y, interleukin-1, monokine induced by interferon-y, interleukin-2 and macrophage inflammatory protein-2 were significantly reduced to control levels with human biofield therapy. CONCLUSION: Human biofield therapy had no significant effect on tumor size or metastasis but produced significant effects on immune responses apparent in the down-regulation of specific lymphocytes and serum cytokines in a mouse breast cancer model.

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