Nagelfar
Bluelight Crew
By which I mean, a drug made that's a ligand which 'neutrally' binds to a site on a receptor, transporter or such; which is separate from the normal active binding conformation/site of another, natural and native ligand to ones own body. But the exogenous molecule's affect is wholly mediated by its chemical reaction to the endogenous molecule when it binds to its usual site of activity.
The example that follows is gleaned from my own limited understanding of how such specific mechanisms may be precluded from actually having such function: and so may be not the best for what I am here trying to convey if possible, but perhaps another may understand what I am trying to get at and have a more viable possibility:
Here's my "example" in the form of a rhetorical question:
If 'nanoparticles' can be used to treat molecules to pass through the blood-brain-barrier, might they also be used to slip molecules from their transporter system without compromising said transporters? (e.g. "compromising" as would be the case in phosphorylation caused by amphetamine on DAT) For instance, a reuptake pump ligand on DAT that doesn't block reuptake but rather alters the DA that crosses, as it crosses, DAT's uptake by said ligand eliciting (or similar) the addition of nanoparticles to each crossing DA molecule when attached to the pump which would impart the ability for DA to freely transport out of DAT immediately. Without thus effecting the other monoamines & also while not effecting DAT itself, but allowing DA to "self-release" on its own volition from that previous influence of an external molecule that is an intrinsically non-toxic ligand to an overlapping site.
The example that follows is gleaned from my own limited understanding of how such specific mechanisms may be precluded from actually having such function: and so may be not the best for what I am here trying to convey if possible, but perhaps another may understand what I am trying to get at and have a more viable possibility:
Here's my "example" in the form of a rhetorical question:
If 'nanoparticles' can be used to treat molecules to pass through the blood-brain-barrier, might they also be used to slip molecules from their transporter system without compromising said transporters? (e.g. "compromising" as would be the case in phosphorylation caused by amphetamine on DAT) For instance, a reuptake pump ligand on DAT that doesn't block reuptake but rather alters the DA that crosses, as it crosses, DAT's uptake by said ligand eliciting (or similar) the addition of nanoparticles to each crossing DA molecule when attached to the pump which would impart the ability for DA to freely transport out of DAT immediately. Without thus effecting the other monoamines & also while not effecting DAT itself, but allowing DA to "self-release" on its own volition from that previous influence of an external molecule that is an intrinsically non-toxic ligand to an overlapping site.
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