Structural Analogs of the GABAkine KRM-II-81 Are Orally Bioavailable Anticonvulsants without Sedation

Kamal P Pandey; Branka Divović; Farjana Rashid; Lalit K Golani; Rok Cerne; Nicolas M Zahn; Michelle Jean Meyer; Leggy A Arnold; Dishary Sharmin; Md Yeunus Mian; Jodi L Smith; Xingjie Ping; Xiaoming Jin; Arnold Lippa; V V N Phani Babu Tiruveedhula; James M Cook; Miroslav M Savić; Jeffrey M Witkin

doi:10.1124/jpet.122.001362

Structural Analogs of the GABAkine KRM-II-81 Are Orally Bioavailable Anticonvulsants without Sedation

J Pharmacol Exp Ther. 2023 Apr;385(1):50-61. doi: 10.1124/jpet.122.001362. Epub 2023 Feb 6.

Authors

Kamal P Pandey^{1

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3

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5}, Branka Divović^{6

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10}, Farjana Rashid^{6

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10}, Lalit K Golani^{6

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10}, Rok Cerne^{6

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8

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10}, Nicolas M Zahn^{6

7

8

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10}, Michelle Jean Meyer^{6

7

8

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10}, Leggy A Arnold^{6

7

8

9

10}, Dishary Sharmin^{6

7

8

9

10}, Md Yeunus Mian^{6

7

8

9

10}, Jodi L Smith^{6

7

8

9

10}, Xingjie Ping^{6

7

8

9

10}, Xiaoming Jin^{6

7

8

9

10}, Arnold Lippa^{6

7

8

9

10}, V V N Phani Babu Tiruveedhula^{6

7

8

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10}, James M Cook^{6

7

8

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10}, Miroslav M Savić^{6

7

8

9

10}, Jeffrey M Witkin^{1

2

3

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5}

Affiliations

¹ Department of Chemistry and Biochemistry, University of Wisconsin-Milwaukee, Milwaukee, Wisconsin (K.P.P., F.R., L.K.G., N.M.Z., M.J.M., L.A.A., D.S., M.Y.M., V.V.N.P.B.T., J.M.C., J.M.W.); kppandey@uwm.edu witkinconsult@gmail.com.
² Department of Pharmacology, Faculty of Pharmacy, University of Belgrade, Belgrade, Serbia (B.D., M.M.S.); kppandey@uwm.edu witkinconsult@gmail.com.
³ Laboratory of Antiepileptic Drug Discovery, St. Vincent's Hospital, Indianapolis, Indiana (R.C., J.L.S., J.M.W.); kppandey@uwm.edu witkinconsult@gmail.com.
⁴ Department of Anatomy and Cell BiologyIndiana University/Purdue University, Indianapolis, Indiana (R.C., X.P., X.J.); kppandey@uwm.edu witkinconsult@gmail.com.
⁵ Faculty of Medicine, University of Ljubljana, Ljubljana, Slovenia (R.C.); and RespireRx Pharmaceuticals Inc., Glen Rock, New Jersey (A.L., J.M.C., J.M.W.) kppandey@uwm.edu witkinconsult@gmail.com.
⁶ Department of Chemistry and Biochemistry, University of Wisconsin-Milwaukee, Milwaukee, Wisconsin (K.P.P., F.R., L.K.G., N.M.Z., M.J.M., L.A.A., D.S., M.Y.M., V.V.N.P.B.T., J.M.C., J.M.W.).
⁷ Department of Pharmacology, Faculty of Pharmacy, University of Belgrade, Belgrade, Serbia (B.D., M.M.S.).
⁸ Laboratory of Antiepileptic Drug Discovery, St. Vincent's Hospital, Indianapolis, Indiana (R.C., J.L.S., J.M.W.).
⁹ Department of Anatomy and Cell BiologyIndiana University/Purdue University, Indianapolis, Indiana (R.C., X.P., X.J.).
¹⁰ Faculty of Medicine, University of Ljubljana, Ljubljana, Slovenia (R.C.); and RespireRx Pharmaceuticals Inc., Glen Rock, New Jersey (A.L., J.M.C., J.M.W.).

Abstract

To provide back-up compounds to support the development of the GABA_A receptor (GABAAR) potentiator KRM-II-81, three novel analogs were designed: replacing the pyridinyl with 2'-Cl-phenyl (FR-II-60), changing the positions of the N and O atoms in the oxazole ring with addition of an ethyl group (KPP-III-34 and KPP-III-51), or substituting a Br atom for the ethynyl of KRM-II-81 (KPP-III-34). The compounds bound to brain GABAARs. Intraperitoneal administration of FR-II-60 and KPP-III-34 produced anticonvulsant activity in mice [maximal electroshock (MES)-induced seizures or 6 Hz-induced seizures], whereas KPP-III-51 did not. Although all compounds were orally bioavailable, structural changes reduced the plasma and brain (FR-II-60 and KPP-III-51) exposures relative to KRM-II-81. Oral administration of each compound produced dose-dependent increases in the latency for both clonic and tonic seizures and the lethality induced by pentylenetetrazol (PTZ) in mice. Since KPP-III-34 produced the highest brain area under the curve (AUC) exposures, it was selected for further profiling. Oral administration of KPP-III-34 suppressed seizures in corneal-kindled mice, hippocampal paroxysmal discharges in mesial temporal lobe epileptic mice, and PTZ-induced convulsions in rats. Only transient sensorimotor impairment was observed in mice, and doses of KPP-III-34 up to 500 mg/kg did not produce impairment in rats. Molecular docking studies demonstrated that all compounds displayed a reduced propensity for binding to α1His102 compared with the sedating compound alprazolam; the bromine-substituted KPP-III-34 achieved the least interaction. Overall, these findings document the oral bioavailability and anticonvulsant efficacy of three novel analogs of KRM-II-81 with reduced sedative effects. SIGNIFICANCE STATEMENT: A new non-sedating compound, KRM-II-81, with reduced propensity for tolerance is moving into clinical development. Three new analogs were orally bioavailable, produced anticonvulsant effects in rodents, and displayed low sensorimotor impairment. KPP-III-34 demonstrated efficacy in models of pharmacoresistant epilepsy. Docking studies demonstrated a low propensity for compound binding to the α1His102 residue implicated in sedation. Thus, three additional structures have been added to the list of non-sedating imidazodiazepine anticonvulsants that could serve as backups in the clinical development of KRM-II-81.

Publication types

Research Support, Non-U.S. Gov't

MeSH terms

Animals
Anticonvulsants* / chemistry
Anticonvulsants* / pharmacology
Anticonvulsants* / therapeutic use
Electroshock
Epilepsy* / drug therapy
Mice
Molecular Docking Simulation
Oxazoles / pharmacology
Pentylenetetrazole
Rats
Receptors, GABA-A / metabolism
Seizures / chemically induced
Seizures / drug therapy

Substances

Anticonvulsants
KRM-II-81
Oxazoles
Receptors, GABA-A
Pentylenetetrazole

Abstract

Publication types

MeSH terms

Substances

Grants and funding