Enhancement of DNA Vaccine Potency Against Legumain

Šmahel, Michal; Dušková, Martina; Poláková, Ingrid; Musil, Jan

doi:10.1097/cji.0000000000000040

Cited by 20 publications

(14 citation statements)

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“…33,48 This observation is just the opposite of the results obtained for DNA vaccination against Aurka, indicating that the nature of the tumor (self-) antigen could play a role in the antitumor effect after depletion of CD25 + cells. 33,48 This observation is just the opposite of the results obtained for DNA vaccination against Aurka, indicating that the nature of the tumor (self-) antigen could play a role in the antitumor effect after depletion of CD25 + cells.…”

Section: Discussionmentioning

confidence: 72%

“…45,46 Using the newly identified H-2K b Aurka 220-228 epitope, we showed that both the PADRE epitope and the LAMP-1 sequences augmented Aurka-specific response after DNA vaccination by means of a gene gun. 47 In our previous studies with the Sox2 48 and legumain self-antigens, 33 we have shown that a single administration of antibody against CD25 before the first DNA vaccination enhanced the activation of splenocytes against both a self-antigen and a helper epitope. These data correspond with our results obtained for the HPV16 E7 antigen.…”

Section: Discussionmentioning

confidence: 94%

“…The PADRE peptide (AKFVAAWTLKAAA; >81% pure), 32 the Lgmn 108-116 peptide derived from mouse legumain (EDVTPENFL; >94% pure), 33 the OVA 257-264 peptide derived from chicken ovalbumin (SINFEKL, >97% pure), 34 the E7 49-57 peptide derived from HPV16 E7 oncoprotein (RAHYNIVTF, > 96% pure), 35 …”

Section: Peptidesmentioning

confidence: 99%

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Combined Cancer Immunotherapy Against Aurora Kinase A

Kaštánková

Poláková

Dušková

et al. 2016

Journal of Immunotherapy

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Aurora kinase A (AURKA) is a centrosomal protein that is overexpressed in a number of human malignancies and can contribute to tumor progression. As we used this protein as a target of DNA immunization, we increased its immunogenicity by the addition of the PADRE helper epitope and decreased its potential oncogenicity by mutagenesis of the kinase domain. For in vitro analysis of induced immune responses in mice, we identified the Aurka(220-228) nonapeptide representing an H-2Kb epitope. As DNA vaccination against the Aurka self-antigen by a gene gun did not show any antitumor effect, we combined DNA immunization with anti-CD25 treatment that depletes mainly regulatory T cells. Whereas 1 anti-CD25 dose injected before DNA vaccination did not enhance the activation of Aurka-specific splenocytes, 3 doses administered on days of immunizations augmented about 10-fold immunity against Aurka. However, an opposite effect was found for antitumor immunity-only 1 anti-CD25 dose combined with DNA vaccination reduced tumor growth. Moreover, the administration of 3 doses of anti-CD25 antibody alone accelerated tumor growth. Analysis of tumor-infiltrating cells showed that 3 anti-CD25 doses not only efficiently depleted regulatory T cells but also activated helper T cells and CD3(-)CD25(+) cells. Next, we found that blockade of the PD-1 receptor initiated 1 week after the first immunization was necessary for significant inhibition of tumor growth with therapeutic DNA vaccination against Aurka combined with depletion of CD25 cells. Our results suggest that combined cancer immunotherapy should be carefully evaluated to achieve the optimal antitumor effect.

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Section: Discussionmentioning

confidence: 72%

Section: Discussionmentioning

confidence: 94%

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Combined Cancer Immunotherapy Against Aurora Kinase A

Kaštánková

Poláková

Dušková

et al. 2016

Journal of Immunotherapy

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“…This discovery led Smahel and his team to modify the gene sequence of legumain to enhance the efficacy of immunization against legumain. These modifications induced reduced legumain maturation and impaired cellular localization, and resulted in T helper (CD4 + ) and cytotoxic (CD8 + ) lymphocyte-dependent elimination of TAMs (43). …”

Section: Targeting Tams With Chemotherapy or Immunotherapymentioning

confidence: 99%

Reprogramming of Tumor-Associated Macrophages with Anticancer Therapies: Radiotherapy versus Chemo- and Immunotherapies

2017

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Tumor-associated macrophages (TAMs) play a central role in tumor progression, metastasis, and recurrence after treatment. Macrophage plasticity and diversity allow their classification along a M1–M2 polarization axis. Tumor-associated macrophages usually display a M2-like phenotype, associated with pro-tumoral features whereas M1 macrophages exert antitumor functions. Targeting the reprogramming of TAMs toward M1-like macrophages would thus be an efficient way to promote tumor regression. This can be achieved through therapies including chemotherapy, immunotherapy, and radiotherapy (RT). In this review, we first describe how chemo- and immunotherapies can target TAMs and, second, we detail how RT modifies macrophage phenotype and present the molecular pathways that may be involved. The identification of irradiation dose inducing macrophage reprogramming and of the underlying mechanisms could lead to the design of novel therapeutic strategies and improve synergy in combined treatments.

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“…A single-chain peptide bound to the CD206 receptor was attached to nanobodies that can selectively target CD206 + TAMs [ 11 ]. Legumain, a stress protein and a member of the asparagine endopeptidase family, can serve as an efficient therapeutic target when overexpressed in TAMs [ 12 ]. Targeting surface markers such as scavenger receptor A and CD52 by using immunotoxin-conjugated monoclonal antibodies (mAbs) has been investigated in ovarian cancer [ 13 ].…”

Section: Introductionmentioning

confidence: 99%

Tumor-associated macrophages, potential targets for cancer treatment

Zhang

2017

Biomark Res

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The fact that various immune cells, including macrophages, can be found in tumor tissues has long been known. With the introduction of concept that macrophages differentiate into a classically or alternatively activated phenotype, the role of tumor-associated macrophages (TAMs) is now beginning to be elucidated. TAMs act as “protumoral macrophages”, contributing to disease progression. As the relationship between TAMs and malignant tumors becomes clearer, TAMs are beginning to be seen as potential therapeutic targets in these cases. In this review, we will discuss how TAMs can be used as therapeutic targets of cancer in clinics.

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Enhancement of DNA Vaccine Potency Against Legumain

Cited by 20 publications

References 0 publications

Combined Cancer Immunotherapy Against Aurora Kinase A

Combined Cancer Immunotherapy Against Aurora Kinase A

Reprogramming of Tumor-Associated Macrophages with Anticancer Therapies: Radiotherapy versus Chemo- and Immunotherapies

Tumor-associated macrophages, potential targets for cancer treatment

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