Radiomitigation and Tissue Repair Activity of Systemically Administered Therapeutic Peptide TP508 Is Enhanced by PEGylation

McVicar, Scott D.; Rayavara, Kempaiah; Carney, Darrell H.

doi:10.1208/s12248-016-0043-7

Cited by 6 publications

(11 citation statements)

References 39 publications

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“…This study, along with other data, suggests that increased survival following TP508 treatments may be due in part to the agent's effect on vascular endothelial cells. PEGylated TP508 enhanced wound closure after combined injury (8 Gy irradiation and wounding) in CD-1 outbred mice (McVicar et al 2017).…”

Section: Tp508 (Rusalatide Acetate Chrysalin)mentioning

confidence: 95%

A review of radiation countermeasures focusing on injury-specific medicinals and regulatory approval status: part III. Countermeasures under early stages of development along with ‘standard of care’ medicinal and procedures not requiring regulatory approval for use

Singh

Hanlon

Santiago

et al. 2017

International Journal of Radiation Biology

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Despite the significant progress that has been made in this area during the last several years, additional effort is needed in order to push promising new agents, currently under development, through the regulatory pipeline. This pipeline for new promising drugs appears to be unreasonably slow and cumbersome; possible reasons for this inefficiency are briefly discussed. Significant and continued effort needs to be afforded to this research and development area, as to date, there is no approved radioprotector that can be administered prior to high dose radiation exposure. This represents a very significant, unmet medical need and a significant security issue. A large number of agents with potential to interact with different biological targets are under development. In the next few years, several additional radiation countermeasures will likely receive Food and Drug Administration approval, increasing treatment options for victims exposed to unwanted ionizing irradiation.

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Section: Tp508 (Rusalatide Acetate Chrysalin)mentioning

confidence: 95%

A review of radiation countermeasures focusing on injury-specific medicinals and regulatory approval status: part III. Countermeasures under early stages of development along with ‘standard of care’ medicinal and procedures not requiring regulatory approval for use

Singh

Hanlon

Santiago

et al. 2017

International Journal of Radiation Biology

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“…The mean half-lives of conjugated peptides are seen to increase overall as indicated in Table 3. There are, however, a few exceptions observed as in the cases of Fawaz et al (38) and McVicar, Rayavara & Carney (47). Note that the half-life of the control peptide for Fawaz et al came from Tang et al (38).…”

Section: Comparison Of Effect Sizesmentioning

confidence: 95%

Conjugates for use in peptide therapeutics: a systematic review and meta-analysis

Wijesinghe

Kumari

Booth

2021

Preprint

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While peptides can be excellent therapeutics for several conditions, their limited in vivo half-lives have been a major bottleneck in the development of therapeutic peptides. Conjugating the peptide to an inert chemical moiety is a strategy that has repeatedly proven to be successful in extending the half-life of some therapeutics. This systematic review and meta-analysis was conducted to examine the available literature and assess it in an unbiased manner to determine which conjugates, both biological and synthetic, provide the greatest increase in therapeutic peptide half-life. Systematic searches run on PubMed, Scopus and SciFinder databases resulted in 845 studies pertaining to the topic, 16 of these were included in this review after assessment against pre-specified inclusion criteria registered on PROSPERO (#CRD42020222579). The most common reasons for exclusion were non-IV administration and large peptide size. Of the 16 studies that were included, a diverse suite of conjugates that increased half-life from 0.1 h to 33.57 h was identified. Amongst these peptides, the largest increase in half-life was seen when conjugated with glycosaminoglycans. A meta-analysis of studies that contained fatty acid conjugates indicated that acylation contributed to a statistically significant extension of half-life. Additionally, another meta-analysis followed by a sensitivity analysis suggested that conjugation with specifically engineered recombinant peptides might contribute to a more efficient extension of peptide half-life as compared to PEGylation. Moreover, we confirmed that while polyethylene glycol is a good synthetic conjugate, its chain length likely has an impact on its effectiveness in extending half-life. Furthermore, we found that most animal studies do not include as much detail when reporting findings as compared to human studies. Inclusion of additional experimental detail on aspects such as independent assessment and randomization may be an easily accomplished strategy to drive more conjugated peptides towards clinical studies.

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“…Out of these nine agents, only one agent, CBLB502, was identified based on well-characterized receptor as a target (Toll-like receptor-5, TLR5) for a ligand (truncated flagellin, TLR5 ligand) [67]. Several additional agents, such as cytokines and growth factors [62,82], indralin [83,84], tocols [85,86] metformin [87][88][89][90], lipopeptides [91][92][93], anti-ceramide antibody [94][95][96], cellular therapeutic agents [97][98][99][100], TP508 [101][102][103], inhibitors of various pathways [104][105][106], Oltipraz [107], and R-spondin1 [108][109][110] are under development as radiation countermeasures for various sub-syndromes of ARS (Table 3) and most of these agents are being developed following PBDD strategy. There are several agents under advanced development that show considerable promise and, accordingly, may very well receive FDA approval for human use in the near future.…”

Section: Development Of Radiation Countermeasures For Arsmentioning

confidence: 99%

“…TP508/Chrysalin/Rusalatide Tested in murine model of radiation and combined injury (radiation plus wound), mitigates H-ARS as well as GI-ARS Small peptide binding domain of human prothrombin and binds to thrombin receptor, counters chronic hypoxia TBDD/PBDD [101][102][103] Inhibitors of various pathways Several such agents inhibiting various cellular signaling pathways are being investigated. These agents interact with cell surface receptors transmitting various cellular signals which lead to changes at cellular and tissue levels TBDD/PBDD [104][105][106] Oltipraz/synthetic dithiolethione Improved survival of irradiated mice Reduces radiation-induced lipid peroxidation and acid phosphatase and modulated, glutathione and alkaline phosphatase PBDD [107] R-spondin1 A 263 amino acid protein, stimulates the repopulation of GI crypt cells and mitigates radiation-induced GI-ARS A mitogenic factor for GI stem cells, induces Wnt/β-catenin pathway and promotion of GI stem cell regeneration PBDD [108][109][110] ARS: acute radiation syndrome, GI-ARS: Gastrointestinal ARS; H-ARS: Hematopoietic-ARS.…”

Section: Development Of Radiation Countermeasures For Arsmentioning

confidence: 99%

Drug discovery strategies for acute radiation syndrome

Singh

Seed²,

Olabisi

2019

Expert Opinion on Drug Discovery

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Introduction: There are at the minimum two major, quite different approaches to advance drug discovery. The first being the target-based drug discovery (TBDD) approach that is commonly referred to as the molecular approach. The second approach is the phenotype-based drug discovery (PBDD), also known as physiology-based drug discovery or empirical approach. Area covered: The authors discuss, herein, the need for developing radiation countermeasure agents for various sub-syndromes of acute radiation syndromes (ARS) following TBDD and PBDD approaches. With time and continuous advances in radiation countermeasure drug development research, the expectation is to have multiple radiation countermeasure agents for each sub-syndrome made available to radiation exposed victims. Expert opinion: The majority of the countermeasures currently being developed for ARS employ the PBDD approach, while the TBDD approach is clearly under-utilized. In the future, an improved drug development strategy might be a 'hybrid' strategy that is more reliant on TBDD for the initial drug discovery via large-scale screening of potential candidate agents, while utilizing PBDD for secondary screening of those candidates, followed by tertiary analytics phase in order to pinpoint efficacious candidates that target the specific sub-syndromes of ARS.

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Radiomitigation and Tissue Repair Activity of Systemically Administered Therapeutic Peptide TP508 Is Enhanced by PEGylation

Cited by 6 publications

References 39 publications

A review of radiation countermeasures focusing on injury-specific medicinals and regulatory approval status: part III. Countermeasures under early stages of development along with ‘standard of care’ medicinal and procedures not requiring regulatory approval for use

A review of radiation countermeasures focusing on injury-specific medicinals and regulatory approval status: part III. Countermeasures under early stages of development along with ‘standard of care’ medicinal and procedures not requiring regulatory approval for use

Conjugates for use in peptide therapeutics: a systematic review and meta-analysis

Drug discovery strategies for acute radiation syndrome

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