Venous mesenteric ischemia carries high procedural burden and elevated mortality in patients with severe presentation

Small peptides patterned after the N terminus of the synaptosomal protein of 25 kDa, a member of the protein complex implicated in Ca 2ϩ -dependent neuronal exocytosis, inhibit in vitro the release of neuromodulators involved in pain signaling, suggesting an in vivo analgesic activity. Here, we report that compound DD04107 (palmitoyl-EEMQRR-NH 2 ), a 6-mer palmitoylated peptide that blocks the inflammatory recruitment of ion channels to the plasma membrane of nociceptors and the release of calcitonin gene-related peptide from primary sensory neurons, displays potent and long-lasting in vivo antihyperalgesia and antiallodynia in chronic models of inflammatory and neuropathic pain, such as the complete Freund's adjuvant, osteosarcoma, chemotherapy, and diabetic neuropathic models. Subcutaneous administration of the peptide produced a dose-dependent antihyperalgesic and antiallodynic activity that lasted Ն24 h. The compound showed a systemic distribution, characterized by a bicompartmental pharmacokinetic profile. Safety pharmacology studies indicated that the peptide is largely devoid of side effects and substantiated that the in vivo activity is not caused by locomotor impairment. Therefore, DD04107 is a potent and long-lasting antinociceptive compound that displays a safe pharmacological profile. These findings support the notion that neuronal exocytosis of receptors and neuronal algogens pivotally contribute to chronic inflammatory and neuropathic pain and imply a central role of peptidergic nociceptor sensitization to the pathogenesis of pain.

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Simultaneous online SPE–HPLC–MS/MS analysis of docetaxel, temsirolimus and sirolimus in whole blood and human plasma

Navarrete¹,

Martínez-Alcázar²,

Durán³

et al. 2013

Journal of Chromatography B

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Semi-Mechanistic Model for Neutropenia after High Dose of Chemotherapy in Breast Cancer Patients

et al. 2009

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Population pharmacokinetics meta-analysis of plitidepsin (Aplidin®) in cancer subjects

Nalda-Molina

Valenzuela

Ramon-Lopez

et al. 2008

Cancer Chemother Pharmacol

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The integration of phase I/II pharmacokinetic data demonstrated plitidepsin linear elimination from plasma, dose-proportionality up to 8.0 mg/m(2), and time-independent pharmacokinetics. The distribution to red blood cells can be considered linear at doses lower than 5 mg/m(2) administered as 3-h or longer infusion. No clinically relevant covariates were identified as predictors of plitidepsin pharmacokinetics.

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Population Pharmacokinetic–Pharmacodynamic Analysis of Neutropenia in Cancer Patients Receiving PM00104 (Zalypsis®)

González-Sales¹,

Valenzuela

Pérez-Ruixo³

et al. 2012

Clin Pharmacokinet

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The influence of active secretion processes on intestinal absorption of salbutamol in the rat

Valenzuela

Nácher

Casabó

et al. 2001

European Journal of Pharmaceutics and Biopharmaceutics

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Profile of P‐glycoprotein Distribution in the Rat and Its Possible Influence on the Salbutamol Intestinal Absorption Irocess

Design and Characterization of a Noncompetitive Antagonist of the Transient Receptor Potential Vanilloid Subunit 1 Channel With In Vivo Analgesic and Anti-inflammatory Activity

An Inhibitor of Neuronal Exocytosis (DD04107) Displays Long-Lasting In Vivo Activity against Chronic Inflammatory and Neuropathic Pain

Simultaneous online SPE–HPLC–MS/MS analysis of docetaxel, temsirolimus and sirolimus in whole blood and human plasma

Semi-Mechanistic Model for Neutropenia after High Dose of Chemotherapy in Breast Cancer Patients

Population pharmacokinetics meta-analysis of plitidepsin (Aplidin®) in cancer subjects

Population Pharmacokinetic–Pharmacodynamic Analysis of Neutropenia in Cancer Patients Receiving PM00104 (Zalypsis®)

The influence of active secretion processes on intestinal absorption of salbutamol in the rat

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