Potential Antifibrillatory Agents. N-(ι-Aminoalkoxy)phthalimides1

Nicotinamide Phosphoribosyltransferase Inhibitors, Design, Preparation, and Structure–Activity Relationship. Mette K. Christensen , Kamille D. Erich...
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Experimental Section3

Potential Antifibrillatory Agents. N-(w-Aminoalkoxy)phthalimides' MILTON J. KORNET College o j Pharmacy, University of Kentucky, Lexington, Kentucky 40506 Received September 22, 1965 Oiir interest in drugs which affect the rate and rhythm of the heart has led l i s to prepare a series of X-(a-aminoa1koxy)phthalimides. These compounds are isosteric with the N-(w-aminoalky1)phthalimides which are known antifitirillants.2 One of the

N-(w-Bromoalk0xy)phthalimides.-These compounds were prepared by the previously described procedure4 with the following modifications. The molar ratio of the reactants was changed as follows: N-hydroxyphthalimide (0.1 mole), alkylene bromide (0.25 mole), and triethylamine (0.125 mole). Separation of the Y-( w-bromoa1koxy)phthalimides from the by-product, w,w'-bis(phthalimidooxy)alkanes, was achieved by recrystallization from 705; aqueous ethanol. The w,w'-bis(phtha1imidooxy)alkanes were insoluble in this solvent syst,em. I n this manner, the yields were improved as follows: X-( p-bromoethoxy)phthalimide, 58.15, mp 97-98', lit.4 mp 94-96'; S-(r-bromopropoxy)phthalimide, 55.7$;, mp 72-73". lit,4 mp 60-65": and ?;-(6-brornobutoxy)phthalimide, 59.45;',, mp 71-72', lit.4 mp 7&72O.

TABLE I ~-(w-L~MIXO.lLICOXY)PHTHALIhlIDEHYDROCHLORIDES

-----yo Calcd

Found

221-223

C14HiJ203. HC1

9.44

8.86

2

208-2 12

C14H16?i204. HCl

S.06

8 68

3

2

235-236

CljHigN203' HC1

9.01

8.96

4

2

264-267

C~SH?&T?O~. HC1

8.63

8.64

J

2

222-223.5

C16HmX;203HCl

8.63

8 33

6

2

249-250

C16H20N203.HC1

8.63

8.72

m

2

210-2 12

C18H18N203 HC1

8.08

8.24

F

3

200-202

C17H22X203.HCl

8.27

8.15

n

1

2

2

IMP,

nitrogen---

Formula

NO.

oca

9 10 11 Compound5 1 through 10 were recrystallized from absolute ethanol, 11 from a b d u t e ethanol-ethyl acetate. latter compounds, ?i-[4-(3-methylpiperidino)butyl]phthalimide,~ is reported to be 1.6 times as potent in auricular and 2.5 times as potent in ventricular fibrillation as quinidine, while being only slightly more toxic. The reaction involved in obtaining the title compounds is shown by the following general equation.

( 1 ) This investigation was assisted in part by Grant GB-3331 from the National Science Foundation. (2) (a) K. Hideg and H. 0. Hankovszky, Acta Chim. Acad. Sci. Hung., 99, 391 (1963); ( b ) K. Hideg, L. Szekeres, H. 0. Hankovszky. and J . Prtpp, Biochem. Pharmacal., Suppl., 1 2 , 171 (1963): (0) K. Hideg and H. 0. Hankovszky, J . Med. Chem., 8, 257 (1965).

N-(w-Aminoa1koxy)phthalimide Hydrochlorides.-A typical reaction is described, that for the preparation of ?rT-(&morpholinobut0xy)phthalimide hydrochloride. The melting points and analyses are given in Table I. A solution of Y-(8-bromobutoxy)phthalimide (7.45 g , 0.025 mole) in 50 ml of dry heriezene was treated with morpholine (4.35 g, 0.05 mole) and refluxed for 2 hr. The precipitated morpholine hydrobromide was filtered! and the filtrate was evaporated in vacuo on a water bath. The residue was dissolved in a mixture of absolute ethanol and ether, and dry HC1 was passed in. The precipitated salt was filtered and recrystallized from absolute ethanol and yielded 7.39 g ( 9 3 . 4 5 ) of product, mp 190-192". Acknowledgment.-The author wishes to acknowledge the assistance of Mr. Stephen Bower in preparing some of the inter.mediates. (3) Melting points \!ere determined iising a Fisher-Johns melting point apparatus and are uncorrected. Elemental analyses were performed b y Dr. K u r t Eder, Geneva, Switzerland. (4) L. Bauer and K. S. Suresh. J . Or@. Chem., 28, 1604 (1963).