OCT2013, an ischaemia‐activated antiarrhythmic prodrug, devoid of the systemic side effects of lidocaine

Hesketh, Louise; Sikkel, Markus B.; Mahoney-Sánchez, Laura; Mazzacuva, Francesca; Chowdhury, Rasheda A.; Tzortzis, Konstantinos N.; Firth, John D.; Winter, James; MacLeod, Kenneth T.; Ogrodzinski, Stefan; Wilder, Catherine D. E.; Patterson, Laurence H.; Peters, Nicholas S.; Curtis, Michael J.

doi:10.1111/bph.15764

Cited by 4 publications

(1 citation statement)

References 62 publications

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“…Meanwhile, few dead cells were found in CB/Lid-5 and CB/Lid-10 groups. This phenomenon could be attributed to the side effects of Lid [ 43 ]. The results of Live/dead staining assay were not fully satisfactory.…”

Section: Resultsmentioning

confidence: 99%

One-step fabrication of lidocaine/CalliSpheres® composites for painless transcatheter arterial embolization

et al. 2022

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Background Transcatheter arterial embolization (TAE) is one of the first-line treatments for advanced hepatocellular cancer. The pain caused by TAE is a stark complication, which remains to be prevented by biomedical engineering methods. Methods Herein, a commercial embolic agent CalliSpheres® bead (CB) was functionally modified with lidocaine (Lid) using an electrostatic self-assembly technique. The products were coded as CB/Lid-n (n = 0, 5, 10, corresponding to the relative content of Lid). The chemical compositions, morphology, drug-loading, and drug-releasing ability of CB/Lid-n were comprehensively investigated. The biocompatibility was determined by hemolysis assay, live/dead cell staining assay, CCK8 assay, immunofluorescence (IHC) staining assay and quantitative real-time PCR. The thermal withdrawal latency (TWL) and edema ratio (ER) were performed to evaluate the analgesia of CB/Lid-n using a plantar inflammation model. A series of histological staining, including immunohistochemistry (IL-6, IL-10, TGF-β and Navi1.7) and TUNEL were conducted to reveal the underlying mechanism of anti-tumor effect of CB/Lid-n on a VX2-tumor bearing model. Results Lid was successfully loaded onto the surface of CalliSpheres® bead, and the average diameter of CalliSpheres® bead increased along with the dosage of Lid. CB/Lid-n exhibited desirable drug-loading ratio, drug-embedding ratio, and sustained drug-release capability. CB/Lid-n had mild toxicity towards L929 cells, while triggered no obvious hemolysis. Furthermore, CB/Lid-n could improve the carrageenan-induced inflammation response micro-environment in vivo and in vitro. We found that CB/Lid-10 could selectively kill tumor by blocking blood supply, inhibiting cell proliferation, and promoting cell apoptosis. CB/Lid-10 could also release Lid to relieve post-operative pain, mainly by remodeling the harsh inflammation micro-environment (IME). Conclusions In summary, CB/Lid-10 has relatively good biocompatibility and bioactivity, and it can serve as a promising candidate for painless transcatheter arterial embolization.

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Section: Resultsmentioning

confidence: 99%

One-step fabrication of lidocaine/CalliSpheres® composites for painless transcatheter arterial embolization

et al. 2022

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Automated fabrication of a scalable heart-on-a-chip device by 3D printing of thermoplastic elastomer nanocomposite and hot embossing

Wu,

Xue,

Zhao

et al. 2024

Bioactive Materials

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Electrophysiological Mechanism of Catestatin Antiarrhythmia: Enhancement of I _to , I _K, and I _K1 and Inhibition of I _Ca _‐L in Rat Ventricular Myocytes

Zhang,

Chen,

et al. 2024

JAHA

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Background Cardiovascular disease remains one of the leading causes of death globally. Myocardial ischemia and infarction, in particular, frequently cause disturbances in cardiac electrical activity that can trigger ventricular arrhythmias. We aimed to investigate whether catestatin, an endogenous catecholamine‐inhibiting peptide, ameliorates myocardial ischemia‐induced ventricular arrhythmias in rats and the underlying ionic mechanisms. Methods and Results Adult male Sprague‐Dawley rats were randomly divided into control and catestatin groups. Ventricular arrhythmias were induced by ligation of the left anterior descending coronary artery and electrical stimulation. Action potential, transient outward potassium current, delayed rectifier potassium current, inward rectifying potassium current, and L‐type calcium current ( I Ca‐L ) of rat ventricular myocytes were recorded using a patch‐clamp technique. Catestatin notably reduced ventricular arrhythmia caused by myocardial ischemia/reperfusion and electrical stimulation of rats. In ventricular myocytes, catestatin markedly shortened the action potential duration of ventricular myocytes, which was counteracted by potassium channel antagonists TEACl and 4‐AP, and I Ca‐L current channel agonist Bay K8644. In addition, catestatin significantly increased transient outward potassium current, delayed rectifier potassium current, and inward rectifying potassium current density in a concentration‐dependent manner. Catestatin accelerated the activation and decelerated the inactivation of the transient outward potassium current channel. Furthermore, catestatin decreased I Ca‐L current density in a concentration‐dependent manner. Catestatin also accelerated the inactivation of the I Ca‐L channel and slowed down the recovery of I Ca‐L from inactivation. Conclusions Catestatin enhances the activity of transient outward potassium current, delayed rectifier potassium current, and inward rectifying potassium current, while suppressing the I Ca‐L in ventricular myocytes, leading to shortened action potential duration and ultimately reducing the ventricular arrhythmia in rats.

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OCT2013, an ischaemia‐activated antiarrhythmic prodrug, devoid of the systemic side effects of lidocaine

Cited by 4 publications

References 62 publications

One-step fabrication of lidocaine/CalliSpheres® composites for painless transcatheter arterial embolization

One-step fabrication of lidocaine/CalliSpheres® composites for painless transcatheter arterial embolization

Automated fabrication of a scalable heart-on-a-chip device by 3D printing of thermoplastic elastomer nanocomposite and hot embossing

Electrophysiological Mechanism of Catestatin Antiarrhythmia: Enhancement of I _to , I _K, and I _K1 and Inhibition of I _Ca _‐L in Rat Ventricular Myocytes

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OCT2013, an ischaemia‐activated antiarrhythmic prodrug, devoid of the systemic side effects of lidocaine

Cited by 4 publications

References 62 publications

One-step fabrication of lidocaine/CalliSpheres® composites for painless transcatheter arterial embolization

One-step fabrication of lidocaine/CalliSpheres® composites for painless transcatheter arterial embolization

Automated fabrication of a scalable heart-on-a-chip device by 3D printing of thermoplastic elastomer nanocomposite and hot embossing

Electrophysiological Mechanism of Catestatin Antiarrhythmia: Enhancement of I to , I K, and I K1 and Inhibition of I Ca ‐L in Rat Ventricular Myocytes

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Electrophysiological Mechanism of Catestatin Antiarrhythmia: Enhancement of I _to , I _K, and I _K1 and Inhibition of I _Ca _‐L in Rat Ventricular Myocytes