Valproic acid suppresses cervical cancer tumor progression possibly via activating Notch1 signaling and enhances receptor-targeted cancer chemotherapeutic via activating somatostatin receptor type II

Tsai, Cheguo; Leslie, Juliana; Franko-Tobin, Laura G.; Prasnal, Monica C.; Yang, Tong; Mackey, L. Vienna; Fuselier, Joseph A.; Coy, David H.; Liu, Mingqiu; Chen, Yu; Sun, Lichun

doi:10.1007/s00404-013-2762-7

Cited by 27 publications

(32 citation statements)

References 21 publications

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“…For instance, VPA could act as a tumor suppressor and up-regulate the SSTR2 that is highly expressed in cervical cancer Hela cells. Based on this, VPA and the SSTR2-targeted conjugate COL-SST, used at much lower doses, display a much more synergitic effect on cervical cancer Hela tumor growth than did each single one given at higher doses [7,43]. Similar results were also observed with the treatment of VPA and another conjugate CPT-SST in Hela tumors in xenografts [9].…”

Section: Vpa In Combination With Cytotoxic Peptide-drug Conjugatesmentioning

confidence: 73%

“…It has been observed that the combination of VPA and the GRPR-targeted CPT-BN conjugate additively suppress in vitro cell proliferation in leukemia MOLT-4, Jurkat cells, osteosarcoma U2OS cells, carcinoid BON cells and CNDT2 cells. We also have observed that the combination of VPA and another SSTR2-targeted CPT-SST conjugate could enhance the cell proliferative suppression in various cancer cells, [9,43]. For instance, VPA could act as a tumor suppressor and up-regulate the SSTR2 that is highly expressed in cervical cancer Hela cells.…”

Section: Vpa In Combination With Cytotoxic Peptide-drug Conjugatesmentioning

confidence: 84%

“…VPA has been used in combination therapeutics with various other compounds, some of which are FDA-approved market drugs [7,8]. These combination treatments display more anti-cancer effects compared to each alone [9,42,43], with some under clinical investigations [7,8,42]. For instance, VPA was used in combination with the topoisomerase I inhibitors Camptothecin (CPT), its new analog irinotecan (CPT-11) or CPT conjugates for treating many cancers such as breast cancer, hepatocellular cancer, cervical cancer, lymphoma, thyroid cancer, pancreatic carcinoid, osteosarcoma and ovarian cancer, displaying synergistic in vitro anti-proliferative and in vivo anti-tumor effects [7,9,44].…”

Section: Vpa In Combination With Cytotoxic Agentsmentioning

confidence: 99%

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Anti-Convulsant Drug Valproic Acid in Cancers and in Combination Anti-Cancer Therapeutics

Coy¹

2014

Mod Chem Appl

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The traditional anti-convulsant drug Valproic Acid (VPA) has been found to be involved in suppressing cancer progression while modulating various cancer-associated signaling pathways. In particular, VPA acts as either a Histone Deacetylase (HDAC) inhibitor or a Notch signaling activator in suppressing tumor growth. VPA is less toxic, and by itself, has limited anti-tumor effects. Thus, VPA has been used as an adjuvant in combination with a variety of other anti-cancer agents for many types of cancers. These combination strategies display potential applications in cancer treatments. In particular, VPA could up-regulate certain G Protein-Coupled Receptors (GPCRs) in some cancer cells. Some of these GPCRs are highly expressed naturally in many cancer cells and these characteristics have been applied towards novel enhanced combination therapeutics with VPA and specific receptor-targeted cytotoxic peptide-drug conjugates.

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Section: Vpa In Combination With Cytotoxic Peptide-drug Conjugatesmentioning

confidence: 73%

Section: Vpa In Combination With Cytotoxic Peptide-drug Conjugatesmentioning

confidence: 84%

Section: Vpa In Combination With Cytotoxic Agentsmentioning

confidence: 99%

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Anti-Convulsant Drug Valproic Acid in Cancers and in Combination Anti-Cancer Therapeutics

Coy¹

2014

Mod Chem Appl

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“…Khanim and colleagues performed a clinical study on patients with acute myeloid leukemia (AML) and indicated that their clinical response to VPA was relevant to the in vivo level of histone acetylation, the proapoptotic genes, and the genes associated with apoptosis. Furthermore, the sensitivity of cell lines derived from hematologic neoplasms to VPA was closely correlated with FOSB expression in vitro (Tsai et al 2013). SMAD4 plays various roles in different stages of PCa.…”

Section: Discussionmentioning

confidence: 98%

Valproic acid (VPA) inhibits the epithelial–mesenchymal transition in prostate carcinoma via the dual suppression of SMAD4

Lan

Yuan

Mao

et al. 2015

J Cancer Res Clin Oncol

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“…HDAC inhibition can increase the expression of several genes by accelerating their transcription, which can enhance the innate immune system and lead to suppression of tumor growth. 9,17 VPA alters the expression of various genes involved in the interaction with the cellular immune system, which is known Figure 5. Generation of mouse CIK cells.…”

Section: Discussionmentioning

confidence: 99%

Synergistic effect of cytokine-induced killer cell with valproate inhibits growth of hepatocellular carcinoma cell in a mouse model

Lee

Nam

Chang

et al. 2017

Cancer Biology & Therapy

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Objective: Long-term prognosis of hepatocellular carcinoma (HCC) remains poor owing to the lack of treatment options for advanced HCC. Cytokine-induced killer (CIK) cells are ex vivo expanded T lymphocytes expressing both NK-and T-cell markers. CIK cell therapy alone is insufficient for treating advanced HCC. Thus, this study aimed to determine whether treatment with CIK cells combined with valproic acid (VPA) could provide a synergistic effect to inhibit tumor growth in a mouse model of HCC. Methods: Upregulation of natural killer group 2D (NKG2D) ligands (retinoic acid early inducible 1 [RAE-1], mouse; major histocompatibility complex class I polypeptide-related sequence A [MIC-A], human) were evaluated by FACS. VPA concentrations that did not reduce tumor volume were calculated to avoid VPA cytotoxicity in a C3H mouse model of HCC. CIK cells were generated from mouse splenocytes using interferon gamma, a CD3 monoclonal antibody, and interleukin 2. The potential synergistic effect of CIK cells combined with VPA was evaluated in the mouse model and tissue pathology was investigated. Results: After 40 h of incubation with VPA, RAE-1 and MIC-A expression were increased in 4 HCC cell lines compared with that in control (2.3-fold in MH-134, 2.4-fold in Huh-7, 3.7-fold in SNU-761, and 6.5-fold in SNU-475). The maximal in vivo VPA dosage that showed no significant cytotoxicity compared with control was 10 mg/kg/day. CIK cells were well generated from C3H mouse splenocytes. After 7 d of treatment with CIK cells plus VPA, a synergistic effect was observed on relative tumor volume in the mouse model of HCC. While the relative tumor volume in untreated control mice increased to 11.25, that in the combination treatment group increased to only 5.20 (P D 0.047). Conclusions: The VPA-induced increase in NKG2D ligands expression significantly enhanced the effects of CIK cell therapy in a mouse model of HCC.

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Valproic acid suppresses cervical cancer tumor progression possibly via activating Notch1 signaling and enhances receptor-targeted cancer chemotherapeutic via activating somatostatin receptor type II

Abstract: VPA could not only suppress tumor progression but also provide a novel promising therapeutic choice in combination with a receptor-targeted cytotoxic conjugate via activating the specific receptor.

Cited by 27 publications

References 21 publications

Anti-Convulsant Drug Valproic Acid in Cancers and in Combination Anti-Cancer Therapeutics

Anti-Convulsant Drug Valproic Acid in Cancers and in Combination Anti-Cancer Therapeutics

Valproic acid (VPA) inhibits the epithelial–mesenchymal transition in prostate carcinoma via the dual suppression of SMAD4

Synergistic effect of cytokine-induced killer cell with valproate inhibits growth of hepatocellular carcinoma cell in a mouse model

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