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Research Article | DOI: https://doi.org/10.31579/2640-1053/229
Research and Training Center ‘Physical and Chemical Materials Science’ Under Kyiv Taras Shevchenko University and NAS of Ukraine, Kiev, Ukraine.
*Corresponding Author: Anthony Kodzo-Grey Venyo. Research and Training Center ‘Physical and Chemical Materials Science’ Under Kyiv Taras Shevchenko University and NAS of Ukraine, Kiev, Ukraine.
Citation: Anthony Kodzo-Grey Venyo, (2025), Immunotherapy in the Scenario of Prostate Cancer an Update, J Cancer Research and Cellular Therapeutics, 9(2); DOI:10.31579/2640-1053/229
Copyright: © 2025, Anthony Kodzo-Grey Venyo. This is an open-access article distributed under the terms of the Creative Commons Attribution License, which permits unrestricted use, distribution, and reproduction in any medium, provided the original author and source are credited.
Received: 22 February 2025 | Accepted: 03 March 2025 | Published: 10 March 2025
Keywords: prostate cancer; immunotherapy; sipuleucil-t; ipilimad; combination treatment; immune profile; promising
Over the last few years, immunotherapy had become an important cancer treatment option, and even though the principles of immunotherapy had evolved over many decades, the FDA approvals of sipuleucel-T and ipilimumab had commenced a new wave in immuno-oncology. Despite the current enthusiasm, it is unlikely that any of the immunotherapy treatments alone could dramatically change the outcomes of prostate cancer; nevertheless, combination therapeutic strategies had been more promising and they do provide a reason for optimism. Many completed and ongoing studies have demonstrated that the combination of cancer vaccines or checkpoint inhibitors with different immunotherapy agents, hormonal therapy (enzalutamide), radiotherapy (radium 223), DNA-damaging agents (olaparib), or chemotherapy (docetaxel) could enhance immune responses and induce more dramatic, long-lasting clinical responses without significant toxicity. The goal of prostate cancer immunotherapy does not have to be complete eradication of advanced disease, but instead the return to an immunological equilibrium with an indolent disease state. Further to determining the optimal combination of therapy regimens, efforts are also being made to ascertain to discover biomarkers of immune response. With such concerted efforts, it is expected that the future of immunotherapy in prostate cancer would be brighter in the future than earlier.
Immunotherapy encompasses a wide variety of treatments to engage the immune system to target malignancies. Over recent years, immunotherapy has made a major impact upon therapy of metastatic cancer and has changed the standard of care for many types of neoplasms. Nevertheless, predicting and understanding of responses across tumour types has been a challenge. While some metastatic cancers have demonstrated dramatic responses to immunotherapy, such as melanoma, lung cancer, and renal cell carcinoma, prostate cancer in Prostate Cancer. [1] Nevertheless, small series of prostate cancer patients have demonstrated impressive responses to cellular and immunotherapy. [1,2] Maselli et al. [2] made the ensuing iterations:
The ensuing article contains an update on immunotherapy in malignant neoplasm of the prostate gland including adenocarcinoma of the prostate gland and other cell types of prostate cancer.
To provide an update on immunotherapy of prostate cancer.
Internet databases were searched including Google, Google Scholar, Yahoo, and PUBMED. The search words that were used included: Immunotherapy of prostate cancer; immunotherapy of carcinoma of the prostate gland, immunotherapy of malignant neoplasm of the prostate gland; immunotherapy of prostatic malignant tumour; and immunotherapy of prostatic cancer. One hundred and ten (110) references were identified which were used to write the article which has been divided into two parts: (A) Overview, and (B) Miscellaneous narrations and discussions from some case reports, case series, and studies related to immunotherapy of prostate cancer.
[A] Overview
Definition / General Statements
Immunomodulators
The ensuing summations had been made regarding the class of immunomodulators and their examples: [3]
Class | Example agents |
---|---|
Interleukin | IL-2, IL-7, IL-12. |
Cytokines | Interferons, G-CSF. |
Chemokines | CCL3, CCL26, CXCL7 |
Immunomodulatory imide drugs (ImiDs) | Thalidomide and its analogues (lenalidomide, pomalidomide, and apremilast), BCG vaccine, [12,13] as well as Covid vaccines [3,12,14,15] |
Others | Cytosine phosphate-guanosine, oligodeoxynucleotides, glucans |
Activation immunotherapies – also exist for utilization.
History of Cancer Immunotherapy
Dendritic cell-based pump-priming or vaccination
The current approaches for DC-based vaccination have been mainly based upon antigen loading on in vitro-generated DCs from monocytes or CD34+ cells, then activating them with different TLR ligands, cytokine combinations, and then injecting them back to the patients. The in vivo targeting approaches do comprise of administering specific cytokines (for example, Flt3L, GM-CSF) and THEN targeting the DCs with antibodies to C-type lectin receptors or agonistic antibodies (for example, anti-CD40) which are then conjugated with antigen of interest. Multiple, next-generation anti-CD40 platforms are being actively developed. [3,34] Future approach might target DC subsets based upon their specifically expressed C-type lectin receptors or chemokine-receptors. Another potential approach is stated to be the generation of genetically engineered DCs from induced pluripotent stem cells and utilisation of neo-antigen-loaded DCs for the induction of better clinical outcome. [3,35]
T-cell adoptive transfer
Checkpoint inhibitors
Immune enhancement therapy
Suppression immunotherapies
It had been iterated that immune suppression does dampen an abnormal immune response in autoimmune diseases, or reduces a normal immune response to prevent rejection of transplanted organs or cells. [3]
Immunosuppressive drugs
Immune tolerance
Approaches to therapeutic tolerance induction [3,68,72,73] | |||
Modality | Details | ||
Non-antigen specific | Monoclonal Antibodies | Depleting:
| Non-depleting:
|
Haematopoietic stem cell transplantation | Non-myeloablative | Myeloablative | |
Mesenchymal stem cell transplantation | |||
Regulatory T cell therapy | Non-antigen specific | Antigen-specific | |
Low dose IL-2 to expand regulatory T cells | |||
Microbiome manipulation | |||
Antigen specific | Peptide therapy | Subcutaneous, intradermal, transmucosal (oral, inhaled) Tolerogenic dendritic cells, liposomes and nanoparticles | |
Altered peptide ligands |
Allergen immunotherapy
Helminthic therapies
Other reported studies related to immunotherapy can be found in: [91-98].
[B] Miscellaneous Narrations And Discussions From Some Case Reports, Case Series, And Studies Related To Immunotherapy Of Prrostate Cancer.
Chen et al. [99] made the ensuing iterations:
Chen et al. [99] reported a case of PCa invading the rectum with focal neuroendocrine differentiation, which was characterized by clinical presentations of defecation difficulties and rectal bleeding. A TPE procedure was undertaken, with a whole exome sequencing (WES) assay indicating that the patient had exhibited a high tumour mutation burden (TMB) and high microsatellite instability (MSI-H). Subsequently, the patient received androgen deprivation therapy (ADT) which was combined with adjuvant immunotherapy following the procedure. At his subsequent six-year follow-up, no local or systemic recurrence was observed, and his serum prostate-specific antigen (PSA) level had remained undetectable. Chen et al. [99] made the ensuing conclusions:
Shi et al. [100] made the ensuing iterations:
Shi et al. [100] reported an 82-year-old male patient, who had manifested with interrupted micturition, dysuria, and significant dysuria on November 24, 2014. He underwent trans-urethral resection of the prostate (TURP) and postoperative pathological examination of the prostatic chips showed prostatic adenocarcinoma, and he underwent a SPECT/CT scan which demonstrated multiple bone metastases. In addition, his serum prostate specific antigen (PSA) and free PSA (FPSA) levels were 54.54 μg/mL and 2.63 μg/mL, respectively, at the beginning of his treatment. His main diagnosis was adenocarcinoma of prostate gland and multiple bone metastases. He received 30 cycles of alloreactive CTL (ACTL) immunotherapy regularly. Over the course of his 2-year treatment, he exhibited diminished bone metastasis which was accompanied by a marked reduction of serum PSA and FPSA from 54.54 and 2.63 μg/ml to 0.003 and <0>
Idossa et al. [101] made the ensuing iterations:
Idossa et al. [101] reported an impressive response to IO combination immunotherapy with ipilimumab plus nivolumab (Ipi/nivo) in a patient who had T-NEPC who had failed standard treatment approaches. The patient was manifesting signs of a rapid decline in quality of life despite his serum prostate-specific antigen (PSA) levels remaining undetectable and he had no previous response to standard therapies. The results of the next-generation sequencing DNA analysis demonstrated the presence of intermediary tumour burden, an ATM mutation and a rare SF3B1 (G742D) mutation, and had served as rational for IO therapy in the patient. Idossa et al. [101] concluded that:
Sharan et al. [102] made the ensuing iterations:
Sharan et al. [102] reported a 58 years old Caucasian male, who was diagnosed with prostate carcinoma with GLEASON score 8. The patient had previously been diagnosed with Renal Cell Carcinoma (RCC) in 1996 and he had undergone nephrectomy of the right kidney. He had PET CT scan, which demonstrated multiple intensely PSMA avid lesions which were identified in both lobes of the prostate gland with SUVmax -28.3 and the prostate gland measuring 3.2 × 3.2 cm displaying maximum dimensions. Pathology examination of his prostate biopsy specimens which were obtained by FNAC followed by PETCT confirmed CA Prostate and the diagnosis was further supported by his increased serum PSA level. He underwent personalised Dendritic Cell Immunotherapy APCEDEN regimen of six doses biweekly, in a time frame of 3 months were given both via intravenous and intradermal route. Six months pursuant to completion of APCEDEN, the patient was administered 6 booster shots for 6 months. Progressive remission of carcinoma was observed together with reduction in his PSA and Testosterone levels. He had PET CT scan which demonstrated decline in PSMA avidity by 50% with SUVmax -14.0 and normal size and shape of prostate gland. Sharan et al. [102] made the ensuing discussions, declaration of lessons to learn and conclusions:
Reed-Perino et al. [103] made the ensuing iterations:
Reed-Perino et al. [103] reported a case of a patient with mCRPC harbouring a somatic dMMR who had progressed on pembrolizumab after an initial response. He enrolled on a clinical trial with JNJ-081, a prostate-specific membrane antigen-CD3 bispecific T-cell engager antibody and had experienced a partial response with the course complicated by cytokine release syndrome. On progression, he was re-initiated on pembrolizumab and he experienced an exceptional second response, with his prostate-specific antigen falling from a high level of 20.01 to undetectable level after 6 weeks and his serum PSA LEVEL HAD remained undetectable for more than (>)11 months. Reed-Perino et al. [103] concluded that:
Cabel et al. [104] made the ensuing iterations:
Cabel et al. [104] reported on two patients who had received ipilimumab in these trials and who were still in long-term complete remission with a follow-up of 64 months and 52 months respectively after the commencement of ipilimumab. Immunohistochemical staining for hMLH1, hMSH2, hMSH6 and PMS2 was undertaken on archival prostate biopsy samples from one of the two patients; they exhibited normal protein expression. Interestingly for this patient, a high CD3+ and CD8+ T cell infiltration was identified on archival prostate biopsies as well as Treg FoxP3+ T cells. Cabel et al. [104] concluded that:
Ashraf et al. [105] made the ensuing iterations:
Ashraf et al. [105] reported their findings as follows:
Ashraf et al. [105] concluded that:
Their research article had provided critical insights into the evolving landscape of immunotherapies being tested for PCa and had addressed gaps in oncological research to advance the understanding of PCa.
Schirrmacher et al. [106] reported the case of a patient with hormone-refractory metastatic prostate cancer who had failed standard treatment, but then achieved complete remission ensuing combined therapy with local hyperthermia (LHT), Newcastle disease virus and dendritic cell (DC) vaccination, which was an unusual combination. In August 2005, the patient had undergone a radical prostatectomy. Despite standard treatment, the patient subsequently developed progressive bone metastases and had stopped conventional therapy in June 2007. Commencing in October 2007, he was treated with LHT, oncolytic virotherapy and DC vaccination. His serum prostate-specific antigen (PSA)-levels, with the highest level of 233.8 ng/ml in January 2008, had decreased to 0.8 ng/ml in late February 2008. In March 2008, a reduction in his bone metastases could be identified by positron emission tomography/computed tomography. Since then, his PSA levels had remained low and the patient was doing well. The treatment had induced a long-lasting antitumor memory T-cell response. This possibly had explained the long-term effectiveness of this novel experimental combined treatment approach.
Ferreira Bruzzi Porto et al. [107] made the ensuing iterations:
Ferreira Bruzzi Porto et al. [107] described an impressive response to IO combination immunotherapy with ipilimumab plus nivolumab (Ipi/nivo) in a patient who had T-NEPC and who had failed standard treatment approaches. The patient was demonstrating signs of a rapid decline in quality of life despite his serum prostate-specific antigen levels remaining undetectable and he had no previous response to standard therapies. The results of his next-generation sequencing DNA analysis had demonstrated the presence of intermediary tumour burden, an ATM mutation and a rare SF3B1 (G742D) mutation, and served as rational for IO therapy in this patient. Ferreira Bruzzi Porto et al. [107] concluded that:
Zhang et al. [108] made the ensuing iteration:
Zhang et al. [108] reported a patient with lung and lymph node metastases from prostate epithelioid hemangioendothelioma who had achieved a significant partial response. This was accomplished via alternating nivolumab therapy with ipilimumab and liposomal doxorubicin, resulting in a progression-free-survival more than 6 months up to the time of the report of his case. The treatment was well-tolerated throughout. Zhang et al. [108] made the ensuing conclusions:
Fei et al. [109] made the ensuing iterations:
Fei et al. [109] reported a case of small cell neuroendocrine carcinoma of the prostate gland with multiple metastases, whose disease had rapidly progressed despite receiving EP and second-line systemic chemotherapy. The patient was then administered a combination of anlotinib and tislelizumab. Following this treatment, the patient’s symptoms were controlled, his tumour marker levels had decreased, and his radiology-imaging showed significant improvement. The patient had a progression-free survival time of more than 22 months and he had continued to receive treatment. Fei et al. [109] concluded that:
Rehman et al. [110] made the ensuing iterations:
Rehman et al. [110] undertook a systematic review which collated and synthesized findings of completed Phase III clinical trials administering immunotherapy; a current clinical trial index (2022) of all ongoing Phase I–III clinical trial records that were also formulated. Rehman et al. [110] summarized their discussions as follows:
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To Dear Erin Aust, I would like to express my heartfelt appreciation for the opportunity to have my work published in this esteemed journal. The entire publication process was smooth and well-organized, and I am extremely satisfied with the final result. The Editorial Team demonstrated the utmost professionalism, providing prompt and insightful feedback throughout the review process. Their clear communication and constructive suggestions were invaluable in enhancing my manuscript, and their meticulous attention to detail and dedication to quality are truly commendable. Additionally, the support from the Editorial Office was exceptional. From the initial submission to the final publication, I was guided through every step of the process with great care and professionalism. The team's responsiveness and assistance made the entire experience both easy and stress-free. I am also deeply impressed by the quality and reputation of the journal. It is an honor to have my research featured in such a respected publication, and I am confident that it will make a meaningful contribution to the field.
"I am grateful for the opportunity of contributing to [International Journal of Clinical Case Reports and Reviews] and for the rigorous review process that enhances the quality of research published in your esteemed journal. I sincerely appreciate the time and effort of your team who have dedicatedly helped me in improvising changes and modifying my manuscript. The insightful comments and constructive feedback provided have been invaluable in refining and strengthening my work".
I thank the ‘Journal of Clinical Research and Reports’ for accepting this article for publication. This is a rigorously peer reviewed journal which is on all major global scientific data bases. I note the review process was prompt, thorough and professionally critical. It gave us an insight into a number of important scientific/statistical issues. The review prompted us to review the relevant literature again and look at the limitations of the study. The peer reviewers were open, clear in the instructions and the editorial team was very prompt in their communication. This journal certainly publishes quality research articles. I would recommend the journal for any future publications.
Dear Jessica Magne, with gratitude for the joint work. Fast process of receiving and processing the submitted scientific materials in “Clinical Cardiology and Cardiovascular Interventions”. High level of competence of the editors with clear and correct recommendations and ideas for enriching the article.
We found the peer review process quick and positive in its input. The support from the editorial officer has been very agile, always with the intention of improving the article and taking into account our subsequent corrections.
My article, titled 'No Way Out of the Smartphone Epidemic Without Considering the Insights of Brain Research,' has been republished in the International Journal of Clinical Case Reports and Reviews. The review process was seamless and professional, with the editors being both friendly and supportive. I am deeply grateful for their efforts.
To Dear Erin Aust – Editorial Coordinator of Journal of General Medicine and Clinical Practice! I declare that I am absolutely satisfied with your work carried out with great competence in following the manuscript during the various stages from its receipt, during the revision process to the final acceptance for publication. Thank Prof. Elvira Farina