TY - JOUR
T1 - Nimodipine pharmacokinetics after intraventricular injection of sustained-release nimodipine for subarachnoid hemorrhage
AU - NEWTON Investigators
AU - MacDonald, R. Loch
AU - Hänggi, Daniel
AU - Strange, Poul
AU - Steiger, Hans Jakob
AU - Mocco, J.
AU - Miller, Michael
AU - Mayer, Stephan A.
AU - Hoh, Brian L.
AU - Faleck, Herbert J.
AU - Etminan, Nima
AU - Diringer, Michael N.
AU - Carlson, Andrew P.
AU - Aldrich, Francois
N1 - Funding Information:
Edge Therapeutics, Inc., funded the study. Dr. Macdonald was an employee and Chief Scientific Officer of Edge Therapeutics, Inc. Drs. Hänggi, Mocco, Mayer, Hoh, Etminan, Diringer, Carlson, and Aldrich received consulting fees from Edge Therapeutics for serving on the steering committee for this trial and for advising Edge Therapeutics, Inc. Drs. Mayer and Aldrich are consultants and receive consulting fees from Actelion Pharmaceuticals, Ltd. Dr. Faleck was an employee of Edge Therapeutics. Drs. Strange and Miller are employees of Integrated Medical Development, LLC. Dr. Mocco reports being a consultant to Imperative Care, Cerebrotech, Viseon, Endostream, Rebound Therapeutics, and Vastrax; ownership in Blink TBI, Serenity, NTI, Neurvana, and Cardinal Consulting; and research support from Stryker, Penumbra, Medtronic, and MicroVention.
Publisher Copyright:
© AANS 2021, except where prohibited by US copyright law.
PY - 2021/1
Y1 - 2021/1
N2 - OBJECTIVE The objective of this study was to measure the concentration of nimodipine in CSF and plasma after intraventricular injection of a sustained-release formulation of nimodipine (EG-1962) in patients with aneurysmal subarachnoid hemorrhage (SAH). METHODS Patients with SAH repaired by clip placement or coil embolization were randomized to EG-1962 or oral nimodipine. Patients were classified as grade 2-4 on the World Federation of Neurosurgical Societies grading scale for SAH and had an external ventricular drain inserted as part of their standard of care. Cohorts of 12 patients received 100-1200 mg of EG-1962 as a single intraventricular injection (9 per cohort) or they remained on oral nimodipine (3 per cohort). Plasma and CSF were collected from each patient for measurement of nimodipine concentrations and calculation of maximum plasma and CSF concentration, area under the concentration-time curve from day 0 to 14, and steady-state concentration. RESULTS Fifty-four patients in North America were randomized to EG-1962 and 18 to oral nimodipine. Plasma concentrations increased with escalating doses of EG-1962, remained stable for 14 to 21 days, and were detectable at day 30. Plasma concentrations in the oral nimodipine group were more variable than for EG-1962 and were approximately equal to those occurring at the EG-1962 800-mg dose. CSF concentrations of nimodipine in the EG-1962 groups were 2-3 orders of magnitude higher than in the oral nimodipine group, in which nimodipine was only detected at low concentrations in 10% (21/213) of samples. In the EG-1962 groups, CSF nimodipine concentrations were 1000 times higher than plasma concentrations. CONCLUSIONS Plasma concentrations of nimodipine similar to those achieved with oral nimodipine and lasting for 21 days could be achieved after a single intraventricular injection of EG-1962. The CSF concentrations from EG-1962, however, were at least 2 orders of magnitude higher than those with oral nimodipine. These results supported a phase 3 study that demonstrated a favorable safety profile for EG-1962 but yielded inconclusive efficacy results due to notable differences in clinical outcome based on baseline disease severity.
AB - OBJECTIVE The objective of this study was to measure the concentration of nimodipine in CSF and plasma after intraventricular injection of a sustained-release formulation of nimodipine (EG-1962) in patients with aneurysmal subarachnoid hemorrhage (SAH). METHODS Patients with SAH repaired by clip placement or coil embolization were randomized to EG-1962 or oral nimodipine. Patients were classified as grade 2-4 on the World Federation of Neurosurgical Societies grading scale for SAH and had an external ventricular drain inserted as part of their standard of care. Cohorts of 12 patients received 100-1200 mg of EG-1962 as a single intraventricular injection (9 per cohort) or they remained on oral nimodipine (3 per cohort). Plasma and CSF were collected from each patient for measurement of nimodipine concentrations and calculation of maximum plasma and CSF concentration, area under the concentration-time curve from day 0 to 14, and steady-state concentration. RESULTS Fifty-four patients in North America were randomized to EG-1962 and 18 to oral nimodipine. Plasma concentrations increased with escalating doses of EG-1962, remained stable for 14 to 21 days, and were detectable at day 30. Plasma concentrations in the oral nimodipine group were more variable than for EG-1962 and were approximately equal to those occurring at the EG-1962 800-mg dose. CSF concentrations of nimodipine in the EG-1962 groups were 2-3 orders of magnitude higher than in the oral nimodipine group, in which nimodipine was only detected at low concentrations in 10% (21/213) of samples. In the EG-1962 groups, CSF nimodipine concentrations were 1000 times higher than plasma concentrations. CONCLUSIONS Plasma concentrations of nimodipine similar to those achieved with oral nimodipine and lasting for 21 days could be achieved after a single intraventricular injection of EG-1962. The CSF concentrations from EG-1962, however, were at least 2 orders of magnitude higher than those with oral nimodipine. These results supported a phase 3 study that demonstrated a favorable safety profile for EG-1962 but yielded inconclusive efficacy results due to notable differences in clinical outcome based on baseline disease severity.
KW - Nimodipine
KW - Subarachnoid hemorrhage
KW - Sustained-release formulation
KW - Vascular disorders
UR - http://www.scopus.com/inward/record.url?scp=85081240380&partnerID=8YFLogxK
U2 - 10.3171/2019.9.JNS191366
DO - 10.3171/2019.9.JNS191366
M3 - Article
C2 - 31812149
AN - SCOPUS:85081240380
SN - 0022-3085
VL - 134
SP - 95
EP - 101
JO - Journal of Neurosurgery
JF - Journal of Neurosurgery
IS - 1
ER -