Molecular design of hybrid tumour necrosis factor-alpha. II: The molecular size of polyethylene glycol-modified tumour necrosis factor-alpha affects its anti-tumour potency

Tsutsumi, Yasuo; Tsunoda, Shin‐ichi; Kamada, Haruhiko; Kihira, Tetsunari; Nakagawa, Shinsaku; Kaneda, Yoshihisa; Kanamori, Tatsuyuki; Mayumi, Tadanori

doi:10.1038/bjc.1996.495

Cited by 44 publications

(34 citation statements)

References 19 publications

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“…administration of native TNF-α, PEG-TNF-α or PEG-vcTNF-α are shown in Figure 7. Native TNF-α was rapidly eliminated from the circulation, and its plasma half-life was only 0.31 h (Table 3) which corresponds to that reported previously [32]. In contrast, the plasma clearance of both PEG-TNF-α and PEG-vcTNF-α was markedly decreased relative to that of native TNF-α and their plasma half-lives were 27.23 and 21.22 h, respectively, approximately 85-and 65-fold longer than that of native TNF-α.…”

Section: Pharmacokinetics Studies In Micesupporting

confidence: 69%

“…Additionally, it is well known that macromolecules are accumulated and retained in the tumor tissue much more than in normal tissues, a phenomenon termed the "enhanced permeability and retention (EPR)" effect [35,36]. Many macromolecular anticancer agents, such as synthetic polymer-conjugating drugs, polymeric micelle-containing drugs and others, have been reported accordingly [32,37]. The increased tumor growth inhibition seen here with the TNF-α conjugates might also result from the EPR effect of PEGylation.…”

Section: Discussionmentioning

confidence: 99%

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Linkage with cathepsin B-sensitive dipeptide promotes the in vitro and in vivo anticancer activity of PEGylated tumor necrosis factor-alpha (TNF-α) against murine fibrosarcoma

Dai

et al. 2011

Sci. China Life Sci.

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To improve the pharmacological profile of tumor necrosis factor alpha (TNF-α), we have synthesized a new PEGylated prodrug, PEG-vcTNF-α, using a cathepsin B-sensitive dipeptide (valine-citrulline, vc) to link branched PEG and TNF-α. PEG-modified TNF-α without the dipeptide linker (PEG-TNF-α) and unconjugated TNF-α were also tested as controls. It was found for the first time that TNF-α released from PEG-vcTNF-α was specifically dependent on the presence of cathepsin B. PEG-vcTNF-α induced higher cytotoxicity and greater apoptosis against L929 murine fibrosarcoma cells than PEG-TNF-α. Reversal of these effects by a cathepsin-B inhibitor confirmed that these effects were mediated by cathepsin B-specific release of TNF-α. In vivo pharmacokinetics studies demonstrated that the plasma stability of PEG-vcTNF-α was significantly increased compared to TNF-α. Finally, the improved anticancer efficacy of PEG-vcTNF-α and the distinct activities among the three formulations confirmed the positive contribution of both PEGylation and the dipeptide linkage to the improved drug-like properties of PEG-vcTNF-α. The results here indicate that linking proteins and PEG via the cathepsin B-sensitive dipeptide may be a promising strategy for developing protein therapeutics.

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Section: Pharmacokinetics Studies In Micesupporting

confidence: 69%

Section: Discussionmentioning

confidence: 99%

Linkage with cathepsin B-sensitive dipeptide promotes the in vitro and in vivo anticancer activity of PEGylated tumor necrosis factor-alpha (TNF-α) against murine fibrosarcoma

Dai

et al. 2011

Sci. China Life Sci.

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“…The PEG remains with the Fv whereas most of the toxin (amino acids 280-613) is transported to the endoplasmic reticulum, where it translocates to the cytosol and kills the cell. Usually, the activity of PEGylated proteins decreases with increasing molecular weight of the attached PEG because the steric hindrance caused by the attached PEG increases with the increasing length of the PEG chain (26). However, in this case PEG20K-LMB-2 had almost the same activity as PEG5K-LMB-2.…”

Section: Discussionmentioning

confidence: 94%

Site-specific chemical modification with polyethylene glycol of recombinant immunotoxin anti-Tac(Fv)-PE38 (LMB-2) improves antitumor activity and reduces animal toxicity and immunogenicity

Tsutsumi

Onda

Nagata

et al. 2000

Proc. Natl. Acad. Sci. U.S.A.

202

137

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. To make a PEGylated recombinant immunotoxin with improved therapeutic properties, we prepared a mutant of antiTac(Fv)-PE38 (LMB-2), a recombinant immunotoxin composed of a single-chain Fv fragment of the anti-human Tac monoclonal antibody to the IL-2 receptor ␣ subunit fused to a 38-kDa fragment of Pseudomonas exotoxin. For site-specific PEGylation of LMB-2, one cysteine residue was introduced into the peptide connector (ASGCGPE) between the Fv and the toxin. This mutant LMB-2 (cys1-LMB-2), which retained full cytotoxic activity, was then sitespecifically conjugated with 5 or 20 kDa of polyethylene glycol-maleimide. When compared with unmodified LMB-2, both PEGylated immunotoxins showed similar cytotoxic activities in vitro but superior stability at 37°C in mouse serum, a 5-to 8-fold increase in plasma half-lives in mice, and a 3-to 4-fold increase in antitumor activity. This was accompanied by a substantial decrease in animal toxicity and immunogenicity. Site-specific PEGylation of recombinant immunotoxins may increase their therapeutic potency in humans.Pseudomonas exotoxin ͉ cancer therapy ͉ immunotherapy ͉ pharmacokinetics ͉ liver toxicity

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“…Recombinant human TNF- (17000 kD, 1×10 7 from Biosea Biotechnology Co., Ltd. (Beijing, China) and cell counting kits-8 (CCK-8) were from Dojindo Laboratories (Kumamoto, Japan). Other reagents and solvents used were of analytical grade.…”

Section: Methodsmentioning

confidence: 99%

“…One of such strategies is PEGylation with a permanent linkage, resulting in an effective drug delivery platform [4]. Conjugation of cytokines such as TNF- with PEG has been shown to improve their in vivo stability and their therapeutic effects [5][6][7]. However, the target molecules conjugate randomly with PEG, and several active cysteine residues are unavoidably modified, reducing the biological activity of these polypeptides.…”

mentioning

confidence: 99%

Preparation and evaluation of a new releasable PEGylated tumor necrosis factor-α (TNF-α) conjugate for therapeutic application

Dai

Chen

et al. 2013

Sci. China Life Sci.

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Molecular design of hybrid tumour necrosis factor-alpha. II: The molecular size of polyethylene glycol-modified tumour necrosis factor-alpha affects its anti-tumour potency

Cited by 44 publications

References 19 publications

Linkage with cathepsin B-sensitive dipeptide promotes the in vitro and in vivo anticancer activity of PEGylated tumor necrosis factor-alpha (TNF-α) against murine fibrosarcoma

Linkage with cathepsin B-sensitive dipeptide promotes the in vitro and in vivo anticancer activity of PEGylated tumor necrosis factor-alpha (TNF-α) against murine fibrosarcoma

Site-specific chemical modification with polyethylene glycol of recombinant immunotoxin anti-Tac(Fv)-PE38 (LMB-2) improves antitumor activity and reduces animal toxicity and immunogenicity

Preparation and evaluation of a new releasable PEGylated tumor necrosis factor-α (TNF-α) conjugate for therapeutic application

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