Pharmacokinetics and Pharmacodynamics of Intrathecal Ziconotide in Chronic Pain Patients

Wermeling, Daniel P.; Drass, Michael; Ellis, David; Mayo, Martha; McGuire, Dawn; O’Connell, Damian P.; Hale, Victoria; Chao, Shih-Hui

doi:10.1177/0091270003043006008

Cited by 24 publications

(44 citation statements)

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“…For example, delivery of conotoxins to the intrathecal space could, in principle (on the basis of limited redistribution because of their peptidic nature), avoid side effects resulting from on-target effects at different sites. In addition, once delivered to these compartments, it seems that many conotoxins are surprisingly stable, with half-lives of hours or more, rather than minutes (Wermeling et al, 2003;Kern et al, 2007). For example, a relatively long half-life in cerebrospinal fluid may also account for the extended duration of action observed after intrathecal dosing of Xen2174 (Lewis, 2011).…”

Section: Discussionmentioning

confidence: 99%

Conus Venom Peptide Pharmacology

Lewis¹,

Dutertre²,

Vetter³

et al. 2012

Pharmacol Rev

375

416

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Section: Discussionmentioning

confidence: 99%

Conus Venom Peptide Pharmacology

Lewis¹,

Dutertre²,

Vetter³

et al. 2012

Pharmacol Rev

375

416

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“…The search identified that the Visual Analogue Scale for Pain Intensity (VAS-PI) was used frequently to measure the different severities of pain, and its reliability for assessing chronic pain has been demonstrated in previous studies [14,15]. The VAS-PI score was used as the primary end point in a number of studies assessing the efficacy of IT ziconotide administered in severe chronic pain [16][17][18][19][20] and in this study it was used to define the core HSs into four levels of severity.…”

Section: Literature Reviewmentioning

confidence: 99%

Eliciting health state utilities from the general public for severe chronic pain

et al. 2009

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“…Moreover, another mechanism can theoretically be accountable for drug lifetimes in CSF. Pharmacokinetic studies of ziconotide (MVIIA) in chronic pain patients suggest that the main pathway for ziconotide clearance is the bulk redistribution of CSF (Wermeling et al, 2003). A later study using a canine model came to a similar conclusion for ziconotide clearance (Yaksh et al, 2012).…”

Section: Figurementioning

confidence: 95%

“…Only a limited amount of data is available on the bioavailability and stability of clinically used ziconotide in plasma or CSF (Newcomb et al, 2000;Wermeling et al, 2003;Yaksh et al, 2012). In our study, the proteolytic stability of CVID, CVIE&F and their analogues was investigated in human serum since it incorporates a highly active mixture of proteases that provides a robust 'test' of peptide stability.…”

Section: Figurementioning

confidence: 99%

Effects of arginine 10 to lysine substitution on ω‐conotoxin CVIE and CVIF block of Ca_v2.2 channels

Berecki

Daly

Huang

et al. 2014

British J Pharmacology

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BACKGROUND AND PURPOSEω-Conotoxins CVIE and CVIF (CVIE&F) selectively inhibit Cav2.2 channels and are lead molecules in the development of novel analgesics. At physiological membrane potentials, CVIE&F block of Cav2.2 channels is weakly reversible. To improve reversibility, we designed and synthesized arginine CVIE&F analogues in which arginine was substituted for lysine at position 10 ([R10K]CVIE&F), and investigated their serum stability and pharmacological actions on voltage-gated calcium channels (VGCCs). EXPERIMENTAL APPROACHChanges in peptide structure due to R10K substitution were assessed by NMR. Peptide stability in human serum was analysed by reversed-phase HPLC and MS over a 24 h period. Two-electrode voltage-clamp and whole-cell patch clamp techniques were used to study [R10K]CVIE&F effects on VGCC currents in Xenopus oocytes and rat dorsal root ganglion neurons respectively. KEY RESULTSR10K substitution did not change the conserved ω-conotoxin backbone conformations of CVIE&F nor the ω-conotoxin selectivity for recombinant or native Cav2.2 channels, although the inhibitory potency of [R10K]CVIF was better than that of CVIF. At −80 mV, the R10K chemical modification significantly affected ω-conotoxin−channel interaction, resulting in faster onset kinetics than those of CVIE&F. Heterologous and native Cav2.2 channels recovered better from [R10K]CVIE&F block than CVIE&F. In human serum, the ω-conotoxin half-lives were 6−10 h. CVIE&F and [R10K]CVIE&F were more stable than CVID. CONCLUSIONS AND IMPLICATIONSR10K substitution in CVIE&F significantly alters the kinetics of ω-conotoxin action and improves reversibility without diminishing conotoxin potency and specificity for the Cav2.2 channel and without diminishing the serum stability. These results may help generate ω-conotoxins with optimized kinetic profiles for target binding. AbbreviationsN

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Pharmacokinetics and Pharmacodynamics of Intrathecal Ziconotide in Chronic Pain Patients

Cited by 24 publications

References 0 publications

Conus Venom Peptide Pharmacology

Conus Venom Peptide Pharmacology

Eliciting health state utilities from the general public for severe chronic pain

Effects of arginine 10 to lysine substitution on ω‐conotoxin CVIE and CVIF block of Ca_v2.2 channels

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Pharmacokinetics and Pharmacodynamics of Intrathecal Ziconotide in Chronic Pain Patients

Cited by 24 publications

References 0 publications

Conus Venom Peptide Pharmacology

Conus Venom Peptide Pharmacology

Eliciting health state utilities from the general public for severe chronic pain

Effects of arginine 10 to lysine substitution on ω‐conotoxin CVIE and CVIF block of Cav2.2 channels

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Product

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About

Effects of arginine 10 to lysine substitution on ω‐conotoxin CVIE and CVIF block of Ca_v2.2 channels