The study aimed to assess the impact of immunotherapy in 368 patients with stage IV breast cancer. The patients were divided into two groups: one receiving a combination of DC-CIK immunotherapy after low-dose chemotherapy, and the other receiving chemotherapy alone (the control group).
The results showed that the DC-CIK immunotherapy led to improved immune function and decreased the risk of disease progression, resulting in increased overall survival. These findings suggest that DC-CIK immunotherapy could be a promising and effective approach for managing tumor growth in patients with stage IV breast cancer.
A study evaluated the effect of immunotherapy in 368 stage IV breast cancer patients. Patients were divided into treatment (DC-CIK immunotherapy after low-dose chemotherapy) and control (chemotherapy alone) groups. DC-CIK therapy enhanced immune function and reduced the risk of disease progression with increased overall survival. The study suggests that DC-CIK immunotherapy could be an effective approach for controlling tumor growth in stage IV breast cancer patients.
Dendritic cells (DCs) and cytokine-induced killer (CIK) cells have both shown activity as immunotherapy in some malignancies. Our aim was to prospective assess the effect of this immunotherapy in patients with stage IV breast cancer. Between Aug 2003 and Dec 2013, we collected 368 patients who met inclusion criteria and divided into immunotherapy group (treatment group: 188 patients) and chemotherapy group (control group: 180 patients). DCs were prepared from the mononuclear cells isolated from patients in the treatment group using IL-2/GM-CSF and were loaded with tumour antigens; CIK cells were prepared by incubating peripheral blood lymphocytes with IL-2, IFN-γ, and CD3 antibodies. After the patients had received low-dose chemotherapy, those in the treatment group also received the DC-CIK therapy, which was repeated four times in a fortnight to form one cycle. At least three cycles of DC-CIK therapy were given. Immune function was measured in treatment group patients’ sera. Disease-free survival (DFS) and Overall survival (OS) after the diagnosis of stage IV breast cancer was assessed after a 10-year follow-up. The result demonstrated that immune function is obviously enhanced after DC-CIK therapy. By Cox regression analysis, DC-CIK therapy reduced the risk of disease progression (p<0.01) with an increased OS (p<0.01). After low-dose chemotherapy, active immunization with DC-CIK immunotherapy is a potentially effective approach for the control of tumour growth in stage IV breast cancer patients.
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