Pharmacokinetics and Pharmacokinetic–Pharmacodynamic Correlations of Therapeutic Peptides

Diao, Lei; Meibohm, Bernd

doi:10.1007/s40262-013-0079-0

Cited by 264 publications

(248 citation statements)

References 87 publications

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“…This is in keeping with animal studies that have isolated protein adducts and found them to generally range from about 50,000 to more than 100,000 Da [14]. Such high molecular weight proteins do not undergo significant glomerular filtration or other forms of renal clearance [15]. Furthermore, 68 % of 557 urine samples contained no quantifiable APAP-CYS, even when serum adduct concentrations were as high as 16.99 μM (Fig.…”

Section: Discussionsupporting

confidence: 83%

Prolonged Acetaminophen-Protein Adduct Elimination During Renal Failure, Lack of Adduct Removal by Hemodiafiltration, and Urinary Adduct Concentrations After Acetaminophen Overdose

et al. 2014

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Elevated concentrations of serum acetaminophenprotein adducts, measured as protein-derived acetaminophen-cysteine (APAP-CYS), have been used to support a diagnosis of APAP-induced liver injury when histories and APAP levels are unhelpful. Adducts have been reported to undergo first-order elimination, with a terminal half-life of about 1.6 days. We wondered whether renal failure would affect APAP-CYS elimination half-life and whether continuous venovenous hemodiafiltration (CVVHDF), commonly used in liver failure patients, would remove adducts to lower their serum concentrations. Terminal elimination half-lives of serum APAP-CYS were compared between subjects with and without renal failure in a prospective cohort study of 168 adults who had ingested excessive doses of APAP. APAP-CYS concentrations were measured in plasma ultrafiltrate during CVVHDF at times of elevated serum adduct concentrations. Paired samples of urine and serum APAP-CYS concentrations were examined to help understand the potential importance of urinary elimination of serum adducts. APAP-CYS elimination half-life was longer in 15 renal failure subjects than in 28 subjects with normal renal function (41.3±2.2 h versus 26.8±1.1 h [mean ± SEM], respectively, p < 0.001). CVVHDF failed to remove detectable amounts of APAP-CYS in any of the nine subjects studied. Sixty-eight percent of 557 urine samples from 168 subjects contained no detectable APAP-CYS, despite levels in serum up to 16.99 μM. Terminal elimination half-life of serum APAP-CYS was prolonged in patients with renal failure for reasons unrelated to renal urinary adduct elimination, and consideration of prolonged elimination needs to be considered if attempting back-extrapolation of adduct concentrations. CVVHDF did not remove detectable APAP-CYS, suggesting approximate APAP-protein adduct molecular weights≥50,000 Da Toxicol. (2015) 11:169-178 DOI 10.1007 in the minority of instances was most compatible with renal adduct production and protein shedding into urine rather than elimination of serum adducts.

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Section: Discussionsupporting

confidence: 83%

Prolonged Acetaminophen-Protein Adduct Elimination During Renal Failure, Lack of Adduct Removal by Hemodiafiltration, and Urinary Adduct Concentrations After Acetaminophen Overdose

et al. 2014

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“…More recently, we have documented that RERF prevents both uPAR 88-92 -and VEGF-induced angiogenesis in vitro and in vivo (13). However, RERF is expected to have some pharmacokinetic drawbacks as drug candidate, which are common to peptides: they are usually very susceptible to proteolytic degradation in vivo and are rapidly cleared from the circulation in minutes (36). To overcome these drawbacks, we have generated a series of peptide analogues of RERF containing Ca-methyl-a-amino acids, a structural modification used in the past to overcome these limitations (37).…”

Section: Discussionmentioning

confidence: 99%

UPARANT: A Urokinase Receptor–Derived Peptide Inhibitor of VEGF-Driven Angiogenesis with Enhanced Stability and In Vitro and In Vivo Potency

Carriero

Bifulco²,

Minopoli

et al. 2014

Molecular Cancer Therapeutics

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This work is based on previous evidence showing that chemotactic sequence of the urokinase receptor (uPAR [88][89][90][91][92] ) drives angiogenesis in vitro and in vivo in a protease-independent manner, and that the peptide AcArg-Glu-Arg-Phe-NH 2 (RERF) prevents both uPAR 88-92 -and VEGF-induced angiogenesis. New N-acetylated and C-amidated peptide analogues containing a-methyl a-amino acids were designed and synthesized to optimize the biochemical properties for therapeutic applications. Among these, Ac-L-Arg-Aib-L-Arg-D-Ca(Me) Phe-NH 2 , named UPARANT, adopts in solution a turned conformation similar to that found for RERF, is stable to sterilization in 3 mg/mL sealed vials in autoclave for 20 minutes at 120 C, is stable in blood, and displays a long-time resistance to enzymatic proteolysis. UPARANT competes with N-formyl-Met-Leu-Phe (fMLF) for binding to the formyl-peptide receptor, inhibits VEGF-directed endothelial cell migration, and prevents cytoskeletal organization and avb3 activation in endothelial cells exposed to VEGF. In vitro, UPARANT inhibits VEGF-dependent tube formation of endothelial cells at a 100Â lower concentration than RERF. In vivo, UPARANT reduces to the basal level VEGF-dependent capillary sprouts originating from the host vessels that invaded Matrigel sponges implanted in mice, and completely prevents neovascularization induced by subcorneal implantation of pellets containing VEGF in rabbits. Both excellent stability and potency position UPARANT as a promising new therapeutic agent for the control of diseases fueled by excessive angiogenesis, such as cancer and inflammation.

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“…C yclic, stapled, and branched peptides constitute a unique and growing class of biomolecules with promise as therapeutics because of their biostability and resistance to proteolytic digestion in physiological environments [1][2][3][4][5][6][7]. In the context of therapeutics, peptide-based drug candidates display both advantages and disadvantages in comparison to their small molecule counterparts.…”

Section: Introductionmentioning

confidence: 99%

“…Peptides, while frequently less toxic than small molecules when administered intravenously and exhibiting higher selectivity for specific biological functions, do not traverse cell membranes with the ease that small molecules do and are prone to proteolytic degradation [8,9]. However, peptides that are protected from degradation via cyclization or stapling have been shown to exhibit high potency and low toxicity, resulting in more promising candidates for drug administration than their linear counterparts [3][4][5][6][7]. A myriad of nonlinear peptides are found naturally in plants, fungi, and bacteria as well as synthetic ones produced in the laboratory [10][11][12][13][14][15][16][17][18].…”

Section: Introductionmentioning

confidence: 99%

Exploitation of the Ornithine Effect Enhances Characterization of Stapled and Cyclic Peptides

Crittenden

Parker

Jenner

et al. 2016

J. Am. Soc. Mass Spectrom.

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Abstract. A method to facilitate the characterization of stapled or cyclic peptides is reported via an arginine-selective derivatization strategy coupled with MS/MS analysis. Arginine residues are converted to ornithine residues through a deguanidination reaction that installs a highly selectively cleavable site in peptides. Upon activation by CID or UVPD, the ornithine residue cyclizes to promote cleavage of the adjacent amide bond. This Arg-specific process offers a unique strategy for site-selective ring opening of stapled and cyclic peptides. Upon activation of each derivatized peptide, site-specific backbone cleavage at the ornithine residue results in two complementary products: the lactam ring-containing portion of the peptide and the aminecontaining portion. The deguanidination process not only provides a specific marker site that initiates fragmentation of the peptide but also offers a means to unlock the staple and differentiate isobaric stapled peptides.

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Pharmacokinetics and Pharmacokinetic–Pharmacodynamic Correlations of Therapeutic Peptides

Cited by 264 publications

References 87 publications

Prolonged Acetaminophen-Protein Adduct Elimination During Renal Failure, Lack of Adduct Removal by Hemodiafiltration, and Urinary Adduct Concentrations After Acetaminophen Overdose

Prolonged Acetaminophen-Protein Adduct Elimination During Renal Failure, Lack of Adduct Removal by Hemodiafiltration, and Urinary Adduct Concentrations After Acetaminophen Overdose

UPARANT: A Urokinase Receptor–Derived Peptide Inhibitor of VEGF-Driven Angiogenesis with Enhanced Stability and In Vitro and In Vivo Potency

Exploitation of the Ornithine Effect Enhances Characterization of Stapled and Cyclic Peptides

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