Disruption of P‐glycoprotein anticancer drug efflux activity by a small recombinant single‐chain Fv antibody fragment targeted to an extracellular epitope

Haus-Cohen, Maya; Assaraf, Yehuda G.; Binyamin, Liat; Benhar, Itai; Reiter, Yoram

doi:10.1002/ijc.20037

Cited by 15 publications

(8 citation statements)

References 34 publications

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“…7–9 Third, use of antibodies and antibody fragments to target and inhibit drug efflux transporters. 10–12 Fourth, silencing of the gene expression of the drug efflux transporters 13–15 or antiapoptotic proteins, such as BCL2 13,16 using antisense oligonucleotides, siRNA, or micro RNA. Fifth, use of small molecules to suppress non-ABC transporter-mediated resistance.…”

Section: Introductionmentioning

confidence: 99%

Pluronics and MDR Reversal: An Update

2014

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Multidrug resistance (MDR) remains one of the biggest obstacles for effective cancer therapy. Currently there are only few methods that are available clinically that are used to bypass MDR with very limited success. In this review we describe how MDR can be overcome by a simple yet effective approach of using amphiphilic block copolymers. Triblock copolymers of poly(ethylene oxide) (PEO) and poly(propylene oxide) (PPO), arranged in a triblock structure PEOPPO-PEO, Pluronics or “poloxamers”, raised a considerable interest in the drug delivery field. Previous studies demonstrated that Pluronics sensitize MDR cancer cells resulting in increased cytotoxic activity of Dox, paclitaxel, and other drugs by 2–3 orders of magnitude. Pluronics can also prevent the development of MDR in vitro and in vivo. Additionally, promising results of clinical studies of Dox/Pluronic formulation reinforced the need to ascertain a thorough understanding of Pluronic effects in tumors. These effects are extremely comprehensive and appear on the level of plasma membranes, mitochondria, and regulation of gene expression selectively in MDR cancer cells. Moreover, it has been demonstrated recently that Pluronics can effectively deplete tumorigenic intrinsically drug-resistant cancer stem cells (CSC). Interestingly, sensitization of MDR and inhibition of drug efflux transporters is not specific or selective to Pluronics. Other amphiphilic polymers have shown similar activities in various experimental models. This review summarizes recent advances of understanding the Pluronic effects in sensitization and prevention of MDR.

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Section: Introductionmentioning

confidence: 99%

Pluronics and MDR Reversal: An Update

2014

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“…Due to these traits, over-expressed multidrug resistance proteins are excellent targets for antibody mediated cancer targeting. [49,50] (Table 1)…”

Section: Over-expressed Moleculesmentioning

confidence: 99%

Antibodies and their Fragments as Anti-Cancer Agents

Schaedel

Reiter

2006

CPD

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The recent developments in the field of recombinant DNA, protein engineering and cancer biology, have let us gain insight into many cancer-related mechanisms. Moreover, novel techniques have facilitated tools allowing unique distinction between malignantly transformed cells, to regular ones. This understanding has paved the way for the rational design of a new age of pharmaceuticals; monoclonal antibodies and their fragments. Antibodies can select antigens on both a specific and high affinity account, and further implementation of these qualities is used to target cancer cells by specifically identifying exogenous antigens of cancer cell populations. The structure of the antibody provides plasticity resonating from its functional sites. Upon binding to the Fc Receptor on effector cells, the crystallisable fragment (Fc) region elicits the onslaught of Antigen Dependent Cell-mediated Cytotoxicity (ADCC) and the plasma-native Complement Dependent Cytotoxicity (CDC) response and apoptosis. The progenitor form of the antibody can evolve in to a tailored therapeutic molecule with the help of recombinant DNA technology. Recombinant antibodies may be linked to potent toxins or radio-labeled fragments, conferring a high killing capability. Other recombinant techniques such as ADEPT, conjugate the specificity of antibodies to a prodrug-catalytic subunit thus creating a high local concentration of an activated chemotherapeutic. Antibodies can be used to recruit the adaptive immune response by binding the antibody fragment to a recombinant MHC molecule displaying a highly immunogenic peptide. Apart from their therapeutic capabilities antibodies are powerful detection tools as observed in the operating theater in a procedure known as Radio-immuno-guided Surgery (RIGS).

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“…Strategies developed to reverse MDR include the use of pharmacological agents that can interact with one or several ABC transporters, thereby inhibiting their functions, monoclonal antibody directed against a specific ABC transporter, and antisense oligonucleotide or oligodeoxynucleotide ( and Table 2 ). 17 , 24 , 103 , 112 , 113 , 114 , 115 , 116 , 117 , 118 An alternative approach also considered using agents that can inhibit the signaling cascade elements responsible for the enhanced expression of ABC transporters in resistant cancer cells 114 . Certain pharmacological agents have been identified and observed to inhibit the transport activity of P‐gp, MRPs, and BCRP/ABCG2 efflux pumps, increase the intracellular drug accumulation, and reverse MDR in vitro and in vivo , and in certain cases have reached clinical trials.…”

Section: Cancer Therapies Against Locally Advanced and Metastatic Canmentioning

confidence: 99%

Recent Advances on the Molecular Mechanisms Involved in the Drug Resistance of Cancer Cells and Novel Targeting Therapies

Mimeault

Hauke

Karmakar

2007

Clin Pharmacol Ther

154

155

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This review summarizes the recent knowledge obtained on the molecular mechanisms involved in the intrinsic and acquired resistance of cancer cells to current cancer therapies. We describe the cascades that are often altered in cancer cells during cancer progression that may contribute in a crucial manner to drug resistance and disease relapse. The emphasis is on the implication of ATPbinding cassette (ABC) multidrug efflux transporters in drug disposition and antiapoptotic factors, including epidermal growth factor receptor cascades and deregulated enzymes in ceramide metabolic pathways. The altered expression and activity of these signaling elements may have a critical role in the resistance of cancer cells to cytotoxic effects induced by diverse chemotherapeutic drugs and cancer recurrence. Of therapeutic interest, new strategies for reversing the multidrug resistance and developing more effective clinical treatments against the highly aggressive, metastatic, and recurrent cancers, based on the molecular targeting of the cancer progenitor cells and their further differentiated progeny, are also described.Important advances in the development of novel early diagnostic and prognostic methods and therapeutic treatments of cancers using surgical tumor resection, hormonal therapies, radiotherapy, or adjuvant chemotherapy, alone or in combination, have been achieved in past years. [1][2][3][4][5][6][7][8][9][10][11][12][13] This has led to a substantial increase in the cure rate for patients diagnosed in the early stages of localized cancers. For patients diagnosed in the late stages of locally invasive and metastatic cancers, the systemic chemotherapeutic regimens represent one of the principal clinical options. In general, the current chemotherapeutic treatments may contribute to enhancing the time to disease progression, overall survival, and quality of life for patients with advanced and aggressive disease states. Unfortunately, current chemotherapeutic treatments for advanced cancers often result in disease relapse and ultimately lead to the death of the patients. [2][3][4][5][6]9,11,12,[14][15][16][17][18][19] The development of resistance by cancer cells to hormonal therapies, radiotherapy, and chemotherapeutic drugs, which usually occurs during cancer progression and after long-term treatment, still represents a major challenge in the clinical cure of advanced and metastatic cancer forms. Therefore, this underlines the critical importance of establishing Correspondence: M Mimeault or SK Batra (mmimeault@unmc.edu or sbatra@unmc.edu). CONFLICT OF INTERESTThe authors declared no conflict of interest. NIH Public Access NIH-PA Author ManuscriptNIH-PA Author Manuscript NIH-PA Author Manuscript molecular mechanisms involved in the drug disposition and resistance or multidrug resistance (MDR) of cancer cells for improving current therapies against aggressive cancers in the clinics. Numerous works have indicated that the alterations in diverse signaling elements may contribute to high levels of resistance to...

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Disruption of P‐glycoprotein anticancer drug efflux activity by a small recombinant single‐chain Fv antibody fragment targeted to an extracellular epitope

Cited by 15 publications

References 34 publications

Pluronics and MDR Reversal: An Update

Pluronics and MDR Reversal: An Update

Antibodies and their Fragments as Anti-Cancer Agents

Recent Advances on the Molecular Mechanisms Involved in the Drug Resistance of Cancer Cells and Novel Targeting Therapies

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