The light at the end of the tunnel—second generation HPMA conjugates for cancer treatment

Yang, Jiyuan; Kopeček, Jindřich

doi:10.1016/j.cocis.2017.07.003

Cited by 69 publications

(55 citation statements)

References 74 publications

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“…Depending on the final application, different PDI are acceptable. For drug delivery applications, it is crucial to obtain homogeneous conjugates due to dosage issues and reproducibility . However, some industrial applications like enzymatic catalysis do not require homogeneous polymer–enzymes conjugates.…”

Section: Resultsmentioning

confidence: 99%

“…Moreover, all HMPA–drugs conjugates remain either in clinical trials or discarded due to issues like wide molecular weight distribution and heterogenicity of the results. On the one hand, the advantages of HPMA encourages these drawback to be overcome . On the other hand, the conjugation of HPMA copolymers with therapeutic proteins remains poorly explored.…”

Section: Introductionmentioning

confidence: 99%

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Ribonuclease A modification with poly[N‐(2‐hydroxypropyl)methacrylamide] copolymers: new route of synthesis and purification

Sánchez‐Trasviña

Mayolo‐Deloisa

Rito‐Palomares

2020

J of Chemical Tech & Biotech

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BACKGROUND N‐(2‐Hydroxypropyl)methacrylamide (HPMA), a synthetic polymer, has biocompatible features that allow it to be used as a drug carrier and used in drug delivery systems; however, its potential as a protein drug carrier has not been completely exploited. This study provides a new conjugation pathway to obtain HPMA–protein conjugates and, the use of hydrophobic interaction chromatography (HIC) to separate polymer–protein conjugates exploiting the hydrophobicity change on the protein surface due to the conjugation. In this work, Ribonuclease A (RNase A, EC 3.1.27.5), with recognized therapeutic properties, was used as a model protein. RESULTS HPMA was copolymerized with N‐(3‐aminopropyl)methacrylamide (APMA) and then activated with glutaraldehyde. The activation process raises copolymer hydrophobicity. Additionally, the HPMA–RNase A conjugation reaction was carried out at pH 5.1 through reductive amination. At higher copolymer molecular weight (> 50 kDa), the conjugation does not occur whereas molecular weights between 30 and 50 kDa promote the conjugation reaction. The native protein was separated from modified protein using HIC and conjugates with a narrow molecular weight were obtained. CONCLUSIONS RNase A can be conjugated with HPMA–APMA copolymer, activated with glutaraldehyde, through reductive amination. This represents an alternative to previous conjugation reactions. Moreover, the molecular size of the copolymer impacts strongly in the conjugation reaction. The HPMA–RNase A conjugates can be separated employing HIC and, it is possible to obtain conjugates with a narrow molecular weight dispersion. This work proposes a new conjugation pathway and purification process in route to developing chromatographic alternatives to efficiently separate HPMA–protein conjugates. © 2020 Society of Chemical Industry

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Section: Resultsmentioning

confidence: 99%

Section: Introductionmentioning

confidence: 99%

Ribonuclease A modification with poly[N‐(2‐hydroxypropyl)methacrylamide] copolymers: new route of synthesis and purification

Sánchez‐Trasviña

Mayolo‐Deloisa

Rito‐Palomares

2020

J of Chemical Tech & Biotech

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“…were discontinued in 2008 because of lack of efficacy [198]. Other polymeric systems also entered clinical trials ( Table 2).…”

Section: Clinical Data On Cathepsinsmentioning

confidence: 99%

Cathepsin-sensitive nanoscale drug delivery systems for cancer therapy and other diseases

Dheer

Nicolas

Shankar

2019

Advanced Drug Delivery Reviews

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Cathepsins are an important category of enzymes that have attracted great attention for the delivery of drugs to improve the therapeutic outcome of a broad range of nanoscale drug delivery systems. These proteases can be utilized for instance through actuation of polymer-drug conjugates (e.g., triggering the drug release) to bypass limitations of many drug candidates. A substantial amount of work has been witnessed in the design and the evaluation of Cathepsinsensitive drug delivery systems, especially based on the tetra-peptide sequence (Gly-Phe-Leu-Gly, GFLG) which has been extensively used as a spacer that can be cleaved in the presence of Cathepsin B. This Review Article will give an in-depth overview of the design and the biological evaluation of Cathepsin-sensitive drug delivery systems and their application in different pathologies including cancer before discussing Cathepsin B-cleavable prodrugs under clinical trials.

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“…Water soluble N-(2-hydroxypropyl) methacrylamide (HPMA) copolymer is considered to be an excellent drug delivery vehicle for its nonimmunogenicity, nontoxicity, biocompatibility, and multifunctionality. [22][23][24] Hence, in this study, SS20 peptide modified HPMA copolymers were developed to enhance mitochondria accumulation without being trapped in endosomes/lysosomes. Overall, physicochemical characteristics of HPMA copolymers were investigated in detail.…”

Section: Introductionmentioning

confidence: 99%

“…pharmacokinetics study, healthy male BALB/c mice(20-22 g) were randomly divided into two groups (n = 7) and intravenously injected with P-Cy5 and P-Cy5-SS20 (Cy5 equivalent concentration 2.5 mg/ kg). At predetermined time points(1,3,6,12,24, 48, 72, and 96 hours), blood samples (20 μL) were taken from the orbital, and the fluorescence intensity of each sample was measured with a Varioskan Flash (excitation at 642 nm and emission at 662 nm). The blood pharmacokinetic parameters were analyzed using a noncompartmental model with PK Solver software.…”

mentioning

confidence: 99%

Improved mitochondrial targeting effect of HPMA copolymer by SS20 peptide mediation and nonendocytosis pathway

Liu

Xiong

et al. 2018

Journal of Peptide Science

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Mitochondrion plays an important role in executing cell programmed death pathway.Therefore, drugs designed to target mitochondria are supposed to make superior contributions to cancer therapy. However, the problem that drugs or drug delivery systems being sequestrated in endosomes/lysosomes needs to be solved for effective drug delivery. Here, mitochondrial targeting and nonendocytic cell entry peptide SS20 modified HPMA copolymer (P-FITC-SS20) was synthesized. With SS20 peptide modification, the uptake behavior of HPMA copolymers changed remarkably compared with unmodified ones. The internalization of P-FITC-SS20 was not influenced by endocytic inhibitors and temperature. Further, the internalized copolymers were not trapped in endosomes/lysosomes. Although cellular uptake of HPMA copolymer was decreased after SS20 peptide modification, SS20 peptide significantly improved mitochondrial accumulation of HPMA copolymers due to its outstanding mitochondrial targeting ability. Moreover, owing to lower susceptibility to macrophagocyte in blood, P-SS20-Cy5 showed longer blood circulation time and enhanced tumor accumulation. The current study validated that SS20 peptide modification is a promising strategy for mitochondrial targeting drug delivery systems and can be further applied to mitochondria associated diseases to improve therapeutic efficacy.

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The light at the end of the tunnel—second generation HPMA conjugates for cancer treatment

Cited by 69 publications

References 74 publications

Ribonuclease A modification with poly[N‐(2‐hydroxypropyl)methacrylamide] copolymers: new route of synthesis and purification

Ribonuclease A modification with poly[N‐(2‐hydroxypropyl)methacrylamide] copolymers: new route of synthesis and purification

Cathepsin-sensitive nanoscale drug delivery systems for cancer therapy and other diseases

Improved mitochondrial targeting effect of HPMA copolymer by SS20 peptide mediation and nonendocytosis pathway

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