Fundamentals of Medicinal Chemistry

(Brent) #1
act by inhibiting cytochrome P-450 enzymes, in particular those that are essen-

tial for the biosynthesis of ergosterol, the main steroid found in fungual cell

membranes. This is thought to result in an accumulation of 14a-methylated

sterols, such as lanosterol, in the membrane. These sterols are believed to

increase the membrane’s permeability, which allows essential cellular contents

to leak from the cell, causing ireversible damage and cell death. Azoles also

inhibit P-450 oxidases in mammals but far higher concentrations than those

required to treat fungi are usually required.

SAR studies have shown that a weakly basic imidazole or 1,2,4-triazole rings

substituted only at the N-1 position are essential for activity. The substituent

must be lipophilic in character and usually contains one or more five or

six membered ring systems, some of which may be attached by an ether,

secondary amine or thioether group to the carbon chain. The more potent

compounds have two or three aromatic substituents, which are singly or

multiply chlorinated or fluorinated at positions 2, 4 and 6. These nonpolar

structures give the compounds a high degree of lipophilicity, and hence mem-

brane solubility.

7. 2. 1. 2 Allylamines

Allylamines are synthetic derivatives of 3-aminopropene (Table 7.1) developed

from naftifine, the allylamine group appearing to be essential for activity. They

are believed to act by inhibiting squalene epoxidase, the enzyme for the squalene

epoxidation stage in the biosynthesis of ergosterol in the fungal membrane. This

leads to an increase in squalene concentration in the membrane with subsequent

loss of membrane integrity, which allows loss of cell contents to occur.

Tolnaftate, although it is not an allylamine, appears to act in a similar fashion.

However, allylamines do not appear to significantly inhibit the mammalian

cholesterol biosynthesis.

Squalene

Squalene
epoxidase O

O 2 Various steps

Ergosterol

HO

2,3-Oxidosqualene

134 SELECTED EXAMPLES OF DRUG ACTION AT SOME COMMON TARGET AREAS

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