<p>In an attempt to synthesize potent blockers of the
influenza A M2 S31N proton channel with modifications of amantadine, we used MD
simulations and MM-PBSA calculations to project binding modes of compounds <b>2-5,</b> which are analogues of <b>1</b>, a dual blocker. Blocking both the
S31N mutant and the wild type (WT) M2, <b>1
</b>is composed of amantadine linked to an aryl head group, (4-methoxy-2-hydroxy)-benzyl.
Compound <b>6</b>, used as control, has an
3-(thiophenyl)isoxazolyl aryl head group, and selectively blocks M2 S31N (but
not WT) in an aryl head group “out” (i.e. N-ward) binding orientation. We then
tested <b>1</b>-<b>6</b> as anti-virals in cell culture and for M2 binding efficacy with
electrophysiology (EP). The new molecules <b>2-5</b>
have a linker between the adamantane and amino group which can be as small as a
CMe<sub>2</sub> in rimantadine derivative <b>2</b>,
or longer like phenyl in <b>3</b>.
Alternatively, we explored the impact of expanding the diameter of adamantane with
diamantyl or triamantyl in <b>4 </b>and<b> 5</b>, respectively. Antiviral effects
against A/WSN/33 and its M2 WT revertant (M2 N31S) were seen for all six
compounds except for <b>5</b> vs. the
native (S31N) virus and (as predicted from previous studies) <b>6</b> vs. the WT revertant. Compounds <b>1-5, </b>projected to bind<b> </b>in a polar head group “in” (C-ward)
orientation, strongly block<b> </b>proton
currents through M2 WT expressed in voltage-clamped oocytes with fast
association rate constants (k<sub>on</sub>), and slow dissociation rate
constants (k<sub>off</sub>). Surprisingly,<b>
2-5, </b>projected to bind<b> </b>in a
polar head group out orientation, do not effectively block M2 S31N-mediated
proton currents in EP. The results from MD and MM-PBSA calculations suggested
that compounds <b>2</b>-<b>5</b> can be fully effective at blocking
the M2 channel when present. The low degree of blocking in M2 S31N is due to
their kinetics of binding observed in EP, i.e. two orders of magnitude
reduction in k<sub>on </sub>compared to <b>6</b>,
and a fast off rate constant similar to that of <b>6</b>,<b> </b>which is consistent
with<b> </b>steered-MDsimulations. The low
k<sub>on</sub> values can be interpreted from MD simulations, which suggest
distortions to V27 cluster of the M2 S31N caused by the longer (even by one
methylene) hydrophobic segment from adamantane to aryl head group, appropriate
to fit from G34 to V27. The deformations in the N-terminus may be sufficiently
energetic for <b>2-5</b> (compared to <b>6</b>)<b>
</b>to cause the observed low k<sub>on</sub>. <br></p>
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