Administration of heat shock protein 65 inhibits murine melanoma growth in vivo

Yang, Jie; Xie, Yuning; Wang, Huaqian; Yao, Yi; Hou, Jingbo; Ma, Yanju; Zhang, Qing; Xing, Yun; Wu, Jie; Li, Taiming; Zheng, Junnian; Liu, Jingjing; Cao, Ruihua

doi:10.3892/mmr.2012.1167

Cited by 3 publications

(1 citation statement)

References 36 publications

(51 reference statements)

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“…Heat shock proteins also are ubiquitous molecular chaperones involved in posttranslational folding, stability, activation and maturation of many proteins that are essential mediators of signal transduction and cell cycle progression [ 35 , 36 ]. Yang and colleagues showed that melanoma-bearing mice immunized against HSP65 exhibited slow growth of tumors, decreased pulmonary metastasis points and prolonged survival in line with the data shown here [ 37 ]. About calcyclin binding protein, it is highly expressed in several type of cancer, including melanoma [ 38 ].…”

Section: Discussionsupporting

confidence: 84%

Cysteine Proteases from V. cundinamarcensis (C. candamarcensis) Inhibit Melanoma Metastasis and Modulate Expression of Proteins Related to Proliferation, Migration and Differentiation

Lemos

Dittz

Santos

et al. 2018

IJMS

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Previous studies showed that P1G10, a proteolytic fraction from Vasconcellea cundinamarcensis latex, reduced the tumor mass in animals bearing melanoma, increased in vitro DNA fragmentation and decreased cell adhesion. Here, we present some molecular and cellular events related to the antimetastatic effect induced by the CMS-2 fraction derived from P1G10 in metastatic melanoma B16-F10 and melanocyte Melan-a. Using difference gel electrophoresis and mass spectrometry, we identified four proteins overexpressed in tumor cells, all of them related to proliferation, survival, migration and cell invasion, that had their expression normalized upon treatment with CMS-2: nucleophosmin 1, heat shock protein 65, calcyclin binding protein and eukaryotic translation initiation factor 4H. In addition, some antioxidant and glycolytic enzymes show increased expression after exposure to CMS-2, along with an induction of melanogenesis (differentiation marker). The down regulation of cofilin 1, a protein involved in cell motility, may explain the inhibition of cell migration and dendritic-like outgrowth in B16-F10 and Melan-a, observed after CMS-2 treatment. Taken together, it is argued that CMS-2 modulates the expression of proteins related to metastatic development, driving the cell to a more differentiated-like state. These effects support the CMS-2 antimetastatic activity and place this fraction in the category of anticancer agent.

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Section: Discussionsupporting

confidence: 84%

Cysteine Proteases from V. cundinamarcensis (C. candamarcensis) Inhibit Melanoma Metastasis and Modulate Expression of Proteins Related to Proliferation, Migration and Differentiation

Lemos

Dittz

Santos

et al. 2018

IJMS

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Vaccines targeting angiogenesis in melanoma

Zahedipour

Zamani

Jamialahmadi

et al. 2021

European Journal of Pharmacology

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The study ofH. pyloriputative candidate factors for single- and multi-component vaccine development

Mirzaei

Poursina

Moghim

et al. 2017

Critical Reviews in Microbiology

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Helicobacter pylori has grown to colonize inside the stomach of nearly half of the world's population, turning into the most prevalent infections in the universe. Medical care failures noticeably confirm the need for a vaccine to hinder or deal with H. pylori. This review is planned to discuss the most known factors as a vaccine candidate, including single (AhpC, BG, CagA, KatA, Fla, Hsp, HWC, Lpp, LPS, NAP, OMP, OMV, SOD, Tpx, Urease, VacA) and multi-component vaccines. Many promising results in the field of single and multivalent vaccine can be seen, but there is no satisfactory outcome and neither a prophylactic nor a therapeutic vaccine to treat or eradicate the infection in human has been acquired. Hence, selecting suitable antigen is an important factor as an appropriate adjuvant. Taken all together, the development of efficient anti-H. pylori vaccines relies on the fully understanding of the interactions between H. pylori and its host immune system. Therefore, more work should be done on epitope mapping, analysis of molecular structure, and determination of the antigen determinant region as well due to design a vaccine, preferably a multi-component vaccine to elicit specific CD4 T-cell responses that are required for H. pylori vaccine efficacy.

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Administration of heat shock protein 65 inhibits murine melanoma growth in vivo

Cited by 3 publications

References 36 publications

Cysteine Proteases from V. cundinamarcensis (C. candamarcensis) Inhibit Melanoma Metastasis and Modulate Expression of Proteins Related to Proliferation, Migration and Differentiation

Cysteine Proteases from V. cundinamarcensis (C. candamarcensis) Inhibit Melanoma Metastasis and Modulate Expression of Proteins Related to Proliferation, Migration and Differentiation

Vaccines targeting angiogenesis in melanoma

The study ofH. pyloriputative candidate factors for single- and multi-component vaccine development

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