Zoledronic acid and thymosin α1 elicit antitumor immunity against prostate cancer by enhancing tumor inflammation and cytotoxic T cells.
Wang. Sheng S; Huang. Maohua M; Chen. Minfeng M; Sun. Zhiting Z; Jiao. Yubo Y; Ye. Geni G; Pan. Jinghua J; Ye. Wencai W; Zhao. Jianfu J; Zhang. Dongmei D
Key Findings
- ADT combined with ZA and Tα1 improved clinical outcomes in advanced prostate cancer patients, likely due to more Tâcell activity.
- In mouse models, ZAâŻ+âŻTα1 slowed tumor growth, increased infiltration of cytotoxic CD8âș T cells, and promoted a proâinflammatory tumor environment.
- The treatment blocked the MyD88/NFâÎșB pathway in cancer cells (reducing their immune evasion) while activating the same pathway in immune cells, enhancing their antiâtumor function.
Practical Outcomes
- For biohackers, the data suggest Tα1 could act as an immuneâboosting supplement, but its benefits appear strongest when paired with zoledronic acid and hormone therapyâinterventions that require medical supervision. Until safety, dosing, and longâterm effects are clarified, selfâadministration of Tα1 for cancer prevention or performance enhancement remains experimental and should be approached cautiously.
Summary
A study found that adding the peptide thymosinâalphaâ1 (Tα1) to the boneâdrug zoledronic acid (ZA) and standard hormone therapy (ADT) helped men with advanced prostate cancer by boosting immune activity against the tumor. The combo increased cancerâkilling Tâcells and reduced the tumorâs ability to suppress the immune system, leading to slower tumor growth in mice and better outcomes in a small patient review.
Abstract
Advanced or metastatic prostate cancer (PCa) is still an incurable malignancy with high lethality and a poor prognosis. Despite the remarkable success of immunotherapy against many types of cancer, most patients with PCa receive minimal benefit from current immunotherapeutic strategies, because PCa is an immune cold tumor with scarce T-cell infiltration in the tumor microenvironment. The aim of this study was to develop an effective immunotherapeutic approach for immune cold PCa tumors. The therapeutic efficacy of androgen deprivation therapy (ADT) and zoledronic acid (ZA) plus thymosin α1 (Tα1) therapy was analyzed retrospectively in patients with advanced or metastatic PCa. The effects and mechanisms by which ZA and Tα1 regulated the immune functions of PCa cells and immune cells were evaluated by a PCa allograft mouse model, flow cytometric analysis, immunohistochemical and immunofluorescence staining assays, and PCR, ELISA, and Western blot analyses. In this study, clinical retrospective analysis revealed that ADT combined with ZA plus Tα1 improved the therapeutic outcomes of patients with PCa, which might be associated with an enhanced frequency of T cells. ZA and Tα1 treatment synergistically inhibited the growth of androgen-independent PCa allograft tumors, with increased infiltration of tumor-specific cytotoxic CD8<sup>+</sup> T cells and enhanced tumor inflammation. Functionally, ZA and Tα1 treatment relieved immunosuppression in PCa cells, stimulated pro-inflammatory macrophages, and enhanced the cytotoxic function of T cells. Mechanistically, ZA plus Tα1 therapy blocked the MyD88/NF-κB pathway in PCa cells but activated this signaling in macrophages and T cells, altering the tumor immune landscape to suppress PCa progression. These findings uncover a previously undefined role for ZA and Tα1 in inhibiting the disease progression of immune cold PCa tumors by enhancing antitumor immunity and pave the way for the application of ZA plus Tα1 therapy as an immunotherapeutic strategy for treating patients with immunologically unresponsive PCa.
Study Information
pubmed
2023
2023-06-01T00:00:00.000Z
10.1136/jitc-2022-006381
12
34