I've been thinking in the last week about what might be coming next in RC land from China now that so many of their precious cathinones are banned. Hopefully they won't keep pumping out garbage, but I've learned to never underestimate their basic ignorance of drug structure-activity relationships and their willingness to cook 50kg batches of absolutely worthless designer drugs. So I started thinking about what logically will they do now? Probably just make some non-banned very horrible aryl ring substituted cathinone or change it by making the carbon chain even longer (with probably worse and worse drugs being made with every new carbon atom on the chain). Then the question that should have been obvious came to me:
Why don't they make some analog of one of the "winners" they already had like MDPV / a-PVP / a-PPP by substituting on the pyrolidine ring? It'd be cheap and the process would be virtually the same for them. So I came up with some candidates using my limited knowledge of pharmacology & stimulant SARs and some info I found about racetam metabolism (most of which which contain a 2-oxo pyrolidine ring and are fairly non-toxic or so it seems). Here are the ones I could think up:
note: I've just used the a-PVP analog versions, but the idea is the same for MDPV, a-PPP, a-PBP, etc versions.
skeleton: alpha-PVP http://s17.postimg.org/8i79wgvd9/PVP.png
For reference purposes.
Analogs:
2'-oxo-PVP http://s14.postimg.org/w6kxs95mn/PVP_2_oxo.png
aka alpha-(2-oxo)pyrrolidinovalerophenone
3'-oxo-PVP http://s9.postimg.org/b3n8bbi99/PVP_3_oxo.png
I figure this one might not metabolize anything like the 2-oxo above.
PyrroleVP http://s22.postimg.org/sd1dsc4zj/PV_Pyrrole.png
2'-PyrrolineVP http://s14.postimg.org/xh1l9n9vj/PV_2_Pyrroline.png
3'-PyrrolineVP http://s9.postimg.org/fzvggr7sd/PV_3_Pyrroline.png
alpha-(2'-fluoro)PVP http://s16.postimg.org/o6dceh3dv/PVP_2_F.png
alpha-(3'-fluoro)PVP http://s24.postimg.org/fvn97cqyb/PVP_3_F.png
alpha-(2',2'-difluoro)PVP http://s16.postimg.org/qvlx9qd0j/PVP_2_2_DF.png
...and so forth with the fluorine atoms. I imagine, in general, the cost would increase with the number of fluorine atoms added.
IndoleVP http://s15.postimg.org/cv8cdo4qx/PV_Indole.png
This might be getting a little to crazy with the tertiary amino substitution. I expect it wouldn't do much as a psychoactive drug at least at low doses...
2',3'-DihydroindoleVP http://s2.postimg.org/of2b77x9z/PV_2_3_dihydroindole.png
Same as above...
2'-PyrazolineVP http://s13.postimg.org/4xcx3wo9x/PV_2_Pyrazoline.png
AzetidineVP http://s23.postimg.org/81up74lnt/PV_Azetidine.png
AziPV
AzetideneVP http://s27.postimg.org/a3x5vd0n5/PV_Azetidene.png
AzePV
Beta-lactamVP http://s7.postimg.org/ul5rbp7jd/PV_Beta_lactam.png
Does anybody here with some pharmacology knowledge have any thoughts on which of these if any we might see next and if they'll be any good or just an new flood of trash that's a far cry away from their PV parent molecules? And do you figure these would not be better drugs than analogs which are substituted at other parts of the molecule? Also is anyone aware of the any of the above molecules being studied or even existing before?
Why don't they make some analog of one of the "winners" they already had like MDPV / a-PVP / a-PPP by substituting on the pyrolidine ring? It'd be cheap and the process would be virtually the same for them. So I came up with some candidates using my limited knowledge of pharmacology & stimulant SARs and some info I found about racetam metabolism (most of which which contain a 2-oxo pyrolidine ring and are fairly non-toxic or so it seems). Here are the ones I could think up:
note: I've just used the a-PVP analog versions, but the idea is the same for MDPV, a-PPP, a-PBP, etc versions.
skeleton: alpha-PVP http://s17.postimg.org/8i79wgvd9/PVP.png
For reference purposes.
Analogs:
2'-oxo-PVP http://s14.postimg.org/w6kxs95mn/PVP_2_oxo.png
aka alpha-(2-oxo)pyrrolidinovalerophenone
3'-oxo-PVP http://s9.postimg.org/b3n8bbi99/PVP_3_oxo.png
I figure this one might not metabolize anything like the 2-oxo above.
PyrroleVP http://s22.postimg.org/sd1dsc4zj/PV_Pyrrole.png
2'-PyrrolineVP http://s14.postimg.org/xh1l9n9vj/PV_2_Pyrroline.png
3'-PyrrolineVP http://s9.postimg.org/fzvggr7sd/PV_3_Pyrroline.png
alpha-(2'-fluoro)PVP http://s16.postimg.org/o6dceh3dv/PVP_2_F.png
alpha-(3'-fluoro)PVP http://s24.postimg.org/fvn97cqyb/PVP_3_F.png
alpha-(2',2'-difluoro)PVP http://s16.postimg.org/qvlx9qd0j/PVP_2_2_DF.png
...and so forth with the fluorine atoms. I imagine, in general, the cost would increase with the number of fluorine atoms added.
IndoleVP http://s15.postimg.org/cv8cdo4qx/PV_Indole.png
This might be getting a little to crazy with the tertiary amino substitution. I expect it wouldn't do much as a psychoactive drug at least at low doses...
2',3'-DihydroindoleVP http://s2.postimg.org/of2b77x9z/PV_2_3_dihydroindole.png
Same as above...
2'-PyrazolineVP http://s13.postimg.org/4xcx3wo9x/PV_2_Pyrazoline.png
AzetidineVP http://s23.postimg.org/81up74lnt/PV_Azetidine.png
AziPV
AzetideneVP http://s27.postimg.org/a3x5vd0n5/PV_Azetidene.png
AzePV
Beta-lactamVP http://s7.postimg.org/ul5rbp7jd/PV_Beta_lactam.png
Does anybody here with some pharmacology knowledge have any thoughts on which of these if any we might see next and if they'll be any good or just an new flood of trash that's a far cry away from their PV parent molecules? And do you figure these would not be better drugs than analogs which are substituted at other parts of the molecule? Also is anyone aware of the any of the above molecules being studied or even existing before?
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