Promising pharmacological profile of a Kunitz-type inhibitor in murine renal cell carcinoma model

Souza, Jean Gabriel de; Morais, Katia L.P.; Anglès-Cano, Eduardo; Boufleur, Pamela; Mello, Evandro Sobroza de; Maria, Durvanei Augusto; Origassa, Clarice Silvia Taemi; Zampolli, Hamilton de Campos; Câmara, Niels Olsen Saraiva; Berra, Carolina Maria; Bosch, Rosemary Viola; Chudzinski-Tavassi, Ana Marisa

doi:10.18632/oncotarget.11555

Cited by 19 publications

(31 citation statements)

References 32 publications

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“…Our results validated previous uses of Amblyomin-X against several tumor cell lines including skin melanoma [15][16][17][18]42 like ER-stress, Mitochondria-stress, and Apoptosis. It is important to note that the transcriptome results presented herein are the mean cell expression values in the tumor's core, a complex system composed of many distinct normal cells surrounding tumor cells.…”

Section: Discussionsupporting

confidence: 87%

“…This molecule has the ability to inhibit Factor Xa in the blood coagulation cascade and triggers apoptosis by activating its intrinsic pathway in tumor cells [14][15][16] . In previous studies, Amblyomin-X showed more avidity in the recognition of tumor cells, and rapid excretion in healthy murines 17 . We have already shown that Amblyomin-X causes cell death via induction of both endoplasmic reticulum (ER) stress and proteasome inhibition (PI) in renal adenocarcinoma (murine RENCA), in melanoma (murine B16F10 and human SK-MEL-28) 18 , as well as in pancreatic (human Mia-Paca-2) tumor cell lines 17,19,20 .…”

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confidence: 79%

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Modulation of stress and immune response by Amblyomin-X results in tumor cell death in a horse melanoma model

Lichtenstein

Iqbal

Will

et al. 2020

Sci Rep

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We have investigated Amblyomin-X-treated horse melanomas to better understand its mode of action through transcriptome analysis and the in vivo model. Amblyomin-X is a Kunitz-type homologous protein that selectively leads to the death of tumor cells via ER stress and apoptosis, currently under investigation as a new drug candidate for cancer treatment. Melanomas are immunogenic tumors, and a better understanding of the immune responses is warranted. Equine melanomas are spontaneous and not so aggressive as human melanomas are, as this study shows that the in vivo treatment of encapsulated horse melanoma tumors led to a significant reduction in the tumor size or even the complete disappearance of the tumor mass through intratumoral injections of Amblyomin-X. Transcriptome analysis identified ER-and mitochondria-stress, modulation of the innate immune system, apoptosis, and possibly immunogenic cell death activation. Interactome analysis showed that Amblyomin-X potentially interacts with key elements found in transcriptomics. Taken together, Amblyomin-X modulated the tumor immune microenvironment in different ways, at least contributing to induce tumor cell death. Melanoma is a type of cancer arising from the malignant transformation of melanocytes, pigment producing-cells found predominantly in the basal layer of the epidermis and eyes. Cutaneous melanoma is the most aggressive and treatment-resistant form of skin cancer responsible for the vast majority of skin cancer-related deaths in the Caucasian population 1. The global incidence of melanoma continues to increase at an alarming rate, despite decades of public prevention programs in many countries. Around 232,000 new cases of skin cancer were recorded worldwide in 2012, accounting for 1.6% of all new cases of cancer back then, while over 300,000 new cases of melanoma were diagnosed worldwide in 2018, according to the World Cancer Research Foundation 2,3. In Brazil, 1,547 deaths were recorded in 2013 due to melanoma, with around 5,690 new cases reported back then, while around 6,260 new cases were expected due in 2018, according to the National Cancer Institute (INCA) 4. Cutaneous melanoma usually affects a higher proportion of patients, in the age range 40-60 years. They can be treated by surgical excision when detected in the early stage (0, I, II and resectable III), however, in the later stages (unresectable III, IV and recurrent melanoma) the treatment options are chemotherapy, target therapy (BRAF/ MEK pathway inhibitors), immunotherapy (checkpoint blockade CTLA-4 receptor inhibition, PD-1 ↔ PD-L1 axis inhibition, and interferon-gamma immunotherapy), or a combination of them. Death in most patients is caused by metastatic disease which may have evolved from the primary tumor. Therefore, there is a need for new

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Section: Discussionsupporting

confidence: 87%

mentioning

confidence: 79%

Modulation of stress and immune response by Amblyomin-X results in tumor cell death in a horse melanoma model

Lichtenstein

Iqbal

Will

et al. 2020

Sci Rep

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“…The current study describes cellular effects induced by Kunitz-type inhibitor associated with distinct cell motility and proteolysis pericellular biological processes in tumor and endothelial cells. We have demonstrated before that Amblyomin-X has antitumor, antithrombotic and antimetastatic activity [25][26][27][28]. Interestingly, no cytotoxic effect was reported in non-tumor cells, such as fibroblasts.…”

Section: Discussionmentioning

confidence: 99%

“…A recombinant form of this protein was shown to have strong pro-apoptotic activity in various murine and human tumor cells via endoplasmic reticulum stress (ER stress), proteasome inhibition, blockage of autophagy, cell cycle arrest, and aggregosome formation [ 22 – 24 ]. In vivo , we have shown that this inhibitor induces tumor regression and reduction of metastasis[ 25 ]. Furthermore, Amblyomin-X has no toxicity in normal cells and presents low toxicity in healthy animals [ 22 , 24 , 26 ].…”

Section: Introductionmentioning

confidence: 99%

Amblyomin-X, a recombinant Kunitz-type inhibitor, regulates cell adhesion and migration of human tumor cells

Schmidt

Morais

Almeida

et al. 2018

Cell Adhesion & Migration

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In a tumor microenvironment, endothelial cell migration and angiogenesis allow cancer to spread to other organs causing metastasis. Indeed, a number of molecules that are involved in cytoskeleton reorganization and intracellular signaling have been investigated for their effects on tumor cell growth and metastasis. Alongside that, Amblyomin-X, a recombinant Kunitz-type protein, has been shown to reduce metastasis and tumor growth in in vivo experiments. In the present report, we provide a mechanistic insight to these antitumor effects, this is, Amblyomin-X modulates Rho-GTPases and uPAR signaling, and reduces the release of MMPs, leading to disruption of the actin cytoskeleton and decreased cell migration of tumor cell lines. Altogether, our data support a role for Amblyomin-X as a novel potential antitumor drug.

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“…The prolongation of PT and aPTT is reversible [154]. Interestingly, several studies pointed out Amblyomin-X as an anti-cancer molecule in vitro and in vivo [154][155][156][157][158][159][160][161].…”

Section: Factor Xa Inhibitorsmentioning

confidence: 99%

Anticoagulants from Hematophagous

Chudzinski-Tavassi¹,

Faria²,

Flores³

2018

Anticoagulant Drugs

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This chapter will focus on anticoagulant molecules described until now from hematophagous animals. The evolutionary scenario for hematophagous animals is convergent and has resulted on a wide diversity of saliva anticoagulants, substances with platelet antiaggregation action, and also with vase-dilating action. Hematophagous animals such as bloodsuckers (leeches, mosquitoes, and ticks) have developed strategies that specifically target proteinases from the hemostatic system of the animals they feed, thus keeping the blood incoagulable. The saliva of those animals provides a large amount of molecules to modulate the innate immune response of the host and to inhibit blood coagulation in order to facilitate the feeding. Thus, anticoagulants from hematophagous animals represent a very interesting tool for studies ranging from basic research to applications in the therapeutic area, as anticoagulant medication. Several studies have pointed out that anticoagulants from hematophagous can also display non-hemostatic functions as antitumor, bringing new perspectives for the study of these molecules. The comprehension of the multi-faced physiological roles of those new anticoagulants from hematophagous opens new perspectives for therapeutic and biotechnological approaches.

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Promising pharmacological profile of a Kunitz-type inhibitor in murine renal cell carcinoma model

Cited by 19 publications

References 32 publications

Modulation of stress and immune response by Amblyomin-X results in tumor cell death in a horse melanoma model

Modulation of stress and immune response by Amblyomin-X results in tumor cell death in a horse melanoma model

Amblyomin-X, a recombinant Kunitz-type inhibitor, regulates cell adhesion and migration of human tumor cells

Anticoagulants from Hematophagous

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