Encapsulation of anti-carbonic anhydrase IX antibody in hydrogel microspheres for tumor targeting

Takáčová, Martina; Hloušková, Gabriela; Zaťovičová, Miriam; Benej, Martin; Sedlakova, Olga; Kopáček, Juraj; Pastorek, Jaromı́r; Lacı́k, Igor; Pastoreková, Silvia

doi:10.1080/14756366.2016.1177523

Cited by 10 publications

(10 citation statements)

References 42 publications

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“…Lin et al ( 2017 ) also surface functionalized triptolide-loaded liposomes with anti-CA IX antibody to target CA IX-positive human non-small cell lung cancer cells (A549) and A549 tumor spheroids, resulting in the efficient cell apoptosis as compared to free drug and non-targeted liposomes. In a study by Takacova et al ( 2016 ), instead of surface functionalization, the scientists encapsulated the monoclonal antibody M75 into alginate microbeads and sodium alginate-cellulose sulfate-poly(methylene-co-guanidine) based microcapsules to knock down the CA IX expressed by tumor cells.…”

Section: Types Of Nanocarriersmentioning

confidence: 99%

Tumor Microenvironment Targeted Nanotherapy

2018

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Recent developments in nanotechnology have brought new approaches to cancer diagnosis and therapy. While enhanced permeability and retention effect promotes nano-chemotherapeutics extravasation, the abnormal tumor vasculature, high interstitial pressure and dense stroma structure limit homogeneous intratumoral distribution of nano-chemotherapeutics and compromise their imaging and therapeutic effect. Moreover, heterogeneous distribution of nano-chemotherapeutics in non-tumor-stroma cells damages the non-tumor cells, and interferes with tumor-stroma crosstalk. This can lead not only to inhibition of tumor progression, but can also paradoxically induce acquired resistance and facilitate tumor cell proliferation and metastasis. Overall, the tumor microenvironment plays a vital role in regulating nano-chemotherapeutics distribution and their biological effects. In this review, the barriers in tumor microenvironment, its consequential effects on nano-chemotherapeutics, considerations to improve nano-chemotherapeutics delivery and combinatory strategies to overcome acquired resistance induced by tumor microenvironment have been summarized. The various strategies viz., nanotechnology based approach as well as ligand-mediated, redox-responsive, and enzyme-mediated based combinatorial nanoapproaches have been discussed in this review.

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Section: Types Of Nanocarriersmentioning

confidence: 99%

Tumor Microenvironment Targeted Nanotherapy

2018

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“…Indeed, G250, formulated as chimeric IgG1 monoclonal antibody and denominated girentuximab, was the first CA IX inhibitor to enter clinical trials [ 57 ], being actually in Phase III, although it seems that its development has been interrupted due to lack of efficacy [ 58 ]. Thus, no other details will be discussed about this Mab, but Pastorekova’s group [ 59 , 60 ] proposed several interesting approaches based both on antibodies that inhibit the catalytic activity as well as those that target the PG domain of CA IX (and do not inhibit the CO 2 hydrase activity of the enzyme). For example the mouse monoclonal antibody VII/20 was shown to bind to the catalytic domain of CA IX, leading to an efficient receptor-mediated internalization of the antibody-enzyme conjugate, which is the main process that regulates abundance and signaling of cell surface proteins [ 60 ].…”

Section: Antibodies Targeting Ca IX and Xii As Antitumor Agentsmentioning

confidence: 99%

“…This internalization has a considerable impact on immunotherapy and in this particular case elicited significant anticancer effects in a mouse xenograft model of colorectal cancer [ 60 ]. The same group [ 59 ] demonstrated that the monoclonal antibody M75 (targeting the PG domain of CA IX and widely used as a reagent in immune-histochemical studies [ 10 , 17 ]) can be encapsulated into alginate microbeads or microcapsules made of sodium alginate, cellulose sulfate, and poly(methylene-co-guanidine), which afforded a rapid M75 antibody release at pH 6.8 (characteristic of the acidic tumors) compared to pH 7.4 (the physiologic, normal pH) [ 59 ].…”

Section: Antibodies Targeting Ca IX and Xii As Antitumor Agentsmentioning

confidence: 99%

Carbonic Anhydrase Inhibition and the Management of Hypoxic Tumors

Supuran¹

2017

Metabolites

197

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Hypoxia and acidosis are salient features of many tumors, leading to a completely different metabolism compared to normal cells. Two of the simplest metabolic products, protons and bicarbonate, are generated by the catalytic activity of the metalloenzyme carbonic anhydrase (CA, EC 4.2.1.1), with at least two of its isoforms, CA IX and XII, mainly present in hypoxic tumors. Inhibition of tumor-associated CAs leads to an impaired growth of the primary tumors, metastases and reduces the population of cancer stem cells, leading thus to a complex and beneficial anticancer action for this class of enzyme inhibitors. In this review, I will present the state of the art on the development of CA inhibitors (CAIs) targeting the tumor-associated CA isoforms, which may have applications for the treatment and imaging of cancers expressing them. Small molecule inhibitors, one of which (SLC-0111) completed Phase I clinical trials, and antibodies (girentuximab, discontinued in Phase III clinical trials) will be discussed, together with the various approaches used to design anticancer agents with a new mechanism of action based on interference with these crucial metabolites, protons and bicarbonate.

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“…by endocytosis (Javier et al 2008). Targets of PEMC are numerous and include different cancer cells and thrombocytes (Javier et al 2008;Takacova et al 2016). The delivery of PEMC to the target organs or tissue may be achieved by various means including peritoneal injections (De Koker et al 2009;Federici et al 2015).…”

Section: Notably In the Presence Of Lps Neutrophil Activation Bymentioning

confidence: 99%

Encapsulated Hsp70 decreases endotoxin-induced production of ROS and TNFα in human phagocytes

Yurinskaya

Kochetkova

Шабарчина

et al. 2017

Cell Stress and Chaperones

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Human heat shock protein Hsp70 was experimentally inserted into polyelectrolyte microcapsules. Encapsulated recombinant Hsp70 was studied in terms of its effects on neutrophil apoptosis, the production of reactive oxygen species, and the secretion of tumor necrosis factor alpha by promonocytic THP-1 cells. It was found that encapsulated Hsp70 effectively inhibits neutrophil apoptosis, unlike free exogenous protein used in solution. In THP-1 cells, encapsulated and free Hsp70 reduced LPS-induced tumor necrosis factor alpha production with a similar efficiency. Encapsulated Hsp70 reduces LPS-induced reactive oxygen species production by neutrophils in the course of its release from the microcapsules but not as much as free Hsp70. Thus, the polyelectrolyte microcapsules can be used as containers for the effective delivery of Hsp70 to neutrophils and monocytes to significantly improve the functioning of the innate immune system.

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Encapsulation of anti-carbonic anhydrase IX antibody in hydrogel microspheres for tumor targeting

Cited by 10 publications

References 42 publications

Tumor Microenvironment Targeted Nanotherapy

Tumor Microenvironment Targeted Nanotherapy

Carbonic Anhydrase Inhibition and the Management of Hypoxic Tumors

Encapsulated Hsp70 decreases endotoxin-induced production of ROS and TNFα in human phagocytes

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