Delayed Disease Progression after Allogeneic Cell Vaccination in Hormone-Resistant Prostate Cancer and Correlation with Immunologic Variables

Michael, Agnieska; Ball, Graham; Quatan, N; Wushishi, F.; Russell, Nicholas; Whelan, Joe; Chakraborty, Prabir; Leader, David P.; Whelan, Mike; Pandha, Hardev

doi:10.1158/1078-0432.ccr-04-2337

Cited by 112 publications

(102 citation statements)

References 43 publications

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“…Mocellin et al 1 published a comprehensive review of these studies in 2004 (webtables I and II), additional clinical studies have been recently published. 2,[25][26][27][28][29] In RCC, autologous tumor cells were retrovirally modified to secrete granulocyte-macrophage colony stimulating factor. Use of granulocyte-macrophage colony stimulating factor-secreting autologous tumor cells was feasible and safe; after vaccination of RCC patients with advanced disease strong DTH reactions of the skin were observed, together with cellular infiltrates at the injection site as well as occasional immunological and clinical responses.…”

Section: Discussionmentioning

confidence: 99%

Allogeneic gene-modified tumor cells (RCC-26/IL-7/CD80) as a vaccine in patients with metastatic renal cell cancer: a clinical phase-I study

et al. 2010

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Despite novel targeted agents, prognosis of metastatic renal cell cancer (RCC) remains poor, and experimental therapeutic strategies are warranted. Transfection of tumor cells with co-stimulatory molecules and/or cytokines is able to increase immunogenicity. Therefore, in our clinical study, 10 human leukocyte antigen (HLA)-A*0201 + patients with histologicallyconfirmed progressive metastatic clear cell RCC were immunized repetitively over 22 weeks with 2.5-40Â10 6 interleukin (IL)-7/CD80 cotransfected allogeneic HLA-A*0201 + tumor cells (RCC26/IL-7/CD80). Endpoints of the study were feasibility, safety, immunological and clinical responses. Vaccination was feasible and safe. In all, 50% of the patients showed stable disease throughout the study; the median time to progression was 18 weeks. However, vaccination with allogeneic RCC26/IL-7/ CD80 tumor cells was not able to induce TH1-polarized immune responses. A TH2 cytokine profile with increasing amounts of antigen-specific IL-10 secretion was observed in most of the responding patients. Interferon-g secretion by patient lymphocytes upon antigen-specific and non-specific stimulation was substantially impaired, both before and during vaccination, as compared with healthy controls. This is possibly due to profound tumor-induced immunosuppression, which may prevent induction of antitumor immune responses by the gene-modified vaccine. Vaccination in minimal residual disease with concurrent depletion of regulatory cells might be one strategy to overcome this limitation.

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Section: Discussionmentioning

confidence: 99%

Allogeneic gene-modified tumor cells (RCC-26/IL-7/CD80) as a vaccine in patients with metastatic renal cell cancer: a clinical phase-I study

et al. 2010

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“…180 A different allogeneic whole-cell vaccine composed of irradiated prostate cell lines OnyCap23, LNCaP and P4E6 demonstrated a decreased PSA velocity in 11 of 26 patients with HRPC and a longer median TTP (58 weeks), compared with other studies (28 weeks). 185 Another approach using a xenogeneic tissue vaccine has recently been shown to stimulate protective immunity against human PC cells. 186 …”

Section: Whole-tumour Cell Vaccinesmentioning

confidence: 99%

Immunology and immunotherapy approaches for prostate cancer

Elkord

2007

Prostate Cancer Prostatic Dis

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Several mechanisms that impair the immune response to promote tumour progression are reported. These mechanisms aim to reduce the ability of antigen-presenting cells to present antigen and activate naïve T cells to support an active immune response or to create a suppressive environment that induce non-functional tumour-associated antigen-specific T cells. Prostate cancer (PC) alone accounts for 33% of incident cancer cases and about 9% of all cancer-related deaths among men in the USA during 2006. Whereas androgen deprivation has remained the first line of therapy for advanced PC, other therapies are still required due to progression to an androgen-resistant state and eventually loss of control in patients receiving hormonal therapy. Immunotherapy seems to be a promising approach to enhance tumour-specific T-cell responses in different cancers including prostate. More importantly, clinical trials in advanced PC patients have shown that immunotherapy may generate significant clinical responses. Immunology and immunotherapy aspects of PC with focus on prostate-specific antigen will be presented.

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“…Given that the proposed mechanism of action requires that the vaccine will be broken down into its constituent peptides, it follows that the HLA type of the vaccine is of secondary importance, since antigen processing will occur regardless of the patient's tissue-type. Indeed, it could be argued that an HLA mismatch might actually be a more potent vaccine because the host versus graft response, initiated by the presence of 'wrong' HLA molecules, may amplify the reaction [28]. Unfortunately, the encouraging Phase II trials with Canvaxin™ in melanoma [29] have not been followed by positive…”

Section: Whole-cell Vaccinesmentioning

confidence: 99%

“…Multilayer perceptron (MLP) artificial neural networks (ANNs) (Figure 1) have been used to develop predictive numerical models that may discriminate between responders and nonresponders to vaccination based on a range of immunological markers [28]. This approach has led to the development of diagnostic models that have good predictive performance with high specificity and sensitivity for blind data.…”

Section: Multiparametric Data Analysismentioning

confidence: 99%

“…Therefore, immune monitoring of these trials is particularly challenging and must, by definition, include multiple parameters. In a recent Phase IIa trial [28], Onyvax produced a database of 20,000 data points, encompassing some 36 variables (Table 2). The correlation of these multiple parameters is complex and cannot be simplified into a two-dimensional model.…”

Section: Box 2 Onyvax Clinical Trialmentioning

confidence: 99%

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