Genetic vaccines against Ep‐CAM break tolerance to self in a limited subset of subjects: Initial identification of predictive biomarkers

Elia, Leonardo; Mennuni, Carmela; Storto, Mariangela; Podda, Silvia; Calvaruso, Francesco; Salucci, Valentina; Aurisicchio, Luigi; Scarito, Alessia; Ciliberto, Gennaro; Monica, Nicola La; Palombo, Fabio

doi:10.1002/eji.200535514

Cited by 13 publications

(12 citation statements)

References 27 publications

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“…Previous studies have shown successful immunotherapy for tumors in a cross-reaction between the xenogeneic homologues and self-molecules in a mouse model (43). In a recent study, mice vaccinated with Ad-hEp-CAM (epithelial cell adhesion molecule) or Ad-rhEp-CAM were protected from a tumor challenge with MC38-hEp-CAM cells; this showed that the immune response induced against hEp-CAM with both vaccines is sufficient to produce a biological antitumor effect (44). VLPs have the capacity to break self-tolerance to produce antibody responses against self-proteins expressed on them (45).…”

Section: Discussionmentioning

confidence: 92%

Mesothelin is a malignant factor and therapeutic vaccine target for pancreatic cancer

Bharadwaj

Zhang

et al. 2008

Molecular Cancer Therapeutics

141

159

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Given the high fatality rate of pancreatic cancer, an effective treatment for this devastating disease is urgently needed. We have shown that mesothelin expression was higher in human pancreatic cancer cells than in human pancreatic duct epithelial cells, and mesothelin mRNA was substantially overexpressed in 18 of 21 (86%) clinical pancreatic adenocarcinoma specimens when compared with the surrounding normal tissues. However, the biological functions of mesothelin in tumor progression are not clearly understood. Here we studied the effects of mesothelin overexpression in pancreatic cancer cell proliferation and migration in vitro and pancreatic cancer progression in vivo. We found that forced expression of mesothelin significantly increased tumor cell proliferation and migration by 90% and 300%, respectively, and increased tumor volume by 4-fold in the nude mice xenograft model when compared with the vector control cell line. Silencing of mesothelin inhibited cell proliferation and migration in pancreatic cancer cells and ablated tumor progression in vivo. Vaccination with chimeric virus-like particles that contain human mesothelin substantially inhibited tumor progression in C57BL/6J mice. The increases in mesothelin-specific antibodies and CTL activity and the decrease in regulatory T cells correlated with reduced tumor progression and prolonged survival. This study revealed novel functions of mesothelin and suggested a new therapeutic vaccine strategy whereby mesothelin is targeted to control pancreatic cancer progression. [Mol Cancer Ther 2008;7(2):286 -96]

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Section: Discussionmentioning

confidence: 92%

Mesothelin is a malignant factor and therapeutic vaccine target for pancreatic cancer

Bharadwaj

Zhang

et al. 2008

Molecular Cancer Therapeutics

141

159

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“…After 16 h medium was changed, and recombinant lentivirus vectors were harvested 48 h later. FACS analysis was conducted as previously described [15]. …”

Section: Methodsmentioning

confidence: 99%

Growth delay of human bladder cancer cells by Prostate Stem Cell Antigen downregulation is associated with activation of immune signaling pathways

et al. 2010

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BackgroundProstate stem cell antigen (PSCA) is a glycosylphosphatidylinositol (GPI) anchored protein expressed not only in prostate but also in pancreas and bladder cancer as shown by immunohistochemistry and mRNA analysis. It has been targeted by monoclonal antibodies in preclinical animal models and more recently in a clinical trial in prostate cancer patients. The biological role played in tumor growth is presently unknown. In this report we have characterized the contribution of PSCA expression to tumor growth.MethodsA bladder cell line was engineered to express a doxycycline (dox) regulated shRNA against PSCA. To shed light on the PSCA biological role in tumor growth, microarray analysis was carried out as a function of PSCA expression. Expression of gene set of interest was further analyzed by qPCRResultsDown regulation of the PSCA expression was associated with reduced cell proliferation in vitro and in vivo. Mice bearing subcutaneous tumors showed a reduced tumor growth upon treatment with dox, which effectively induced shRNA against PSCA as revealed by GFP expression. Pathway analysis of deregulated genes suggests a statistical significant association between PSCA downregulation and activation of genes downstream of the IFNα/β receptor.ConclusionsThese experiments established for the first time a correlation between the level of PSCA expression and tumor growth and suggest a role of PSCA in counteracting the natural immune response.

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“…One reason for the ability of xenogeneic antigen to break tolerance, as described in the paper in this issue of the European Journal of Immunology by Leonardo et al [8], is likely to be the presence of some foreign sequence in the xenogeneic antigen that is able to activate Th cells; however, this is rather a 'hit and miss' approach to breaking tolerance for therapeutic purposes since the degree of difference between self and xenogeneic antigen is often small and might be sufficient to induce an immune response only in a minority of patients with a suitable MHC Class II background. The variable performance of the mouse Ep-CAM vaccine in outbred mice described in the study by Lenardo et al [8] could reflect this heterogeneity.…”

Section: Importance Of T-cell Helpmentioning

confidence: 99%

“…One of these is electroporation, which has been shown to increase performance in large animals, including rhesus macaques [14]. Leonardo et al [8] use electroporation but combine it with a boost using a viral vector. The latter, however, introduces the problem of immunity against viral proteins which may be pre-existing and can block any boosting [15].…”

Section: Delivery Of Antigenmentioning

confidence: 99%

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Optimizing cancer immunotherapy trials: Back to basics

Stevenson¹,

Rice²

2006

Eur J Immunol

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Attempts to raise effective immunity against cancer are benefiting from information on the nature of the immunity involved and its regulation and, perhaps, now it is time to step back and define our approach in molecular terms prior to clinical testing. Although there are immunological differences between mice and patients, results from murine studies are encouraging early 'translation' of concepts to the clinic and it is vital to take immunological principles emerging from mice into clinical vaccine design. One is the requirement to break tolerance against over-expressed self-antigens, a potentially risky procedure but necessary for several cancer targets. A study in this issue of the European Journal of Immunology attempts to do this by using xenogeneic antigens, albeit with variable outcome. The unstated goal is to activate T-cell help but this can be achieved more effectively by harnessing a predictable anti-microbial repertoire. The second issue lies in the delivery of antigen. One strategy is "prime/boost" using DNA priming and boosting with a viral vector; however, this induces blocking immunity against viral proteins, and must be used judiciously. There are other physical methods to increase immunity such as electroporation, which can itself be used in 'prime/boost' sequence. These twin problems of engagement of T-cell help and delivery of adequate antigen can now be addressed by applying immunological logic to cancer vaccines.See accompanying article http://dx

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Genetic vaccines against Ep‐CAM break tolerance to self in a limited subset of subjects: Initial identification of predictive biomarkers

Cited by 13 publications

References 27 publications

Mesothelin is a malignant factor and therapeutic vaccine target for pancreatic cancer

Mesothelin is a malignant factor and therapeutic vaccine target for pancreatic cancer

Growth delay of human bladder cancer cells by Prostate Stem Cell Antigen downregulation is associated with activation of immune signaling pathways

Optimizing cancer immunotherapy trials: Back to basics

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