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The Large and Nifty Not-quite-advanced Drug Chemistry, Pharmacology and More Thread
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MurphyClox
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With regard to 2C-CN:
I couldn't find any verified data so can only speculate. I'd think the toxicity should approximately be in the range of 2C-B, -C & -D.
Cyanide toxicity is not expected in this case. But lets consider the unlikely (and furthermore unrealistic) scenario of quantitative cyanide-release from 2C-CN for a moment:
Shulgin lists 2-40 mg as common dosage, therefore I will calculate with the median, 30 mg. The molar weight of 2C-CN is 242.7 (as hydrochloride salt), a dose of 30 mg equals therefore 123 µmol. Wikipedia lists the letal dose for cyanide (CN-, not KCN or NaCN) as ca. 140 mg, which equals 5.4 mmol.
Relating these values, one can see that even upon quantitative release of cyanide from 2C-CN, the lethal dose is still 43 times larger.
Ergo: Cyanide poisoning, either with a lethal or sublethal dosage, is far unrealistic both from the metabolic perspective (see my last post above) as well as from the consumed amounts.
Take care!
- Murphy
I couldn't find any verified data so can only speculate. I'd think the toxicity should approximately be in the range of 2C-B, -C & -D.
Cyanide toxicity is not expected in this case. But lets consider the unlikely (and furthermore unrealistic) scenario of quantitative cyanide-release from 2C-CN for a moment:
Shulgin lists 2-40 mg as common dosage, therefore I will calculate with the median, 30 mg. The molar weight of 2C-CN is 242.7 (as hydrochloride salt), a dose of 30 mg equals therefore 123 µmol. Wikipedia lists the letal dose for cyanide (CN-, not KCN or NaCN) as ca. 140 mg, which equals 5.4 mmol.
Relating these values, one can see that even upon quantitative release of cyanide from 2C-CN, the lethal dose is still 43 times larger.
Ergo: Cyanide poisoning, either with a lethal or sublethal dosage, is far unrealistic both from the metabolic perspective (see my last post above) as well as from the consumed amounts.
Take care!
- Murphy
MurphyClox
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1. Synthesis-discussion and even synthesis-related topics are forbidden here!
2. Anyway, to answer in short: Your question is too sketchy to be answered properly.
It really depends on a lot of criteria, for example the reaction's mechanism, solubility of reagents, required reaction temperature, ...
Without further info, there's no answer possible. Well, but adding more details brings us directly back to 1.
![:\](https://bluelight.org/xf/BL_Images/Orig_Emoji/wrygrin.gif "wry grin :\")
- Murphy
Christo_Rey
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Question: bk-MDMA has been patented by Shulgin (1996) as an antidepressant. Is anyone aware of actual clinical trials that were done with it, and where I could read about them?
Don't know if it's the best thread to ask this, but don't know where else to ask.
Don't know if it's the best thread to ask this, but don't know where else to ask.
Clayden's "Organic Chemistry", by a long way
Suggested reading order for Pihkal?
What order should I read Pihkal (part 2) in if I want to read it as a narrative?
That is: everything was cooked up and ingested in a certain order, and that order wasn't alphabetical. Is there a chronological index (or something along those lines) somewhere?
What order should I read Pihkal (part 2) in if I want to read it as a narrative?
That is: everything was cooked up and ingested in a certain order, and that order wasn't alphabetical. Is there a chronological index (or something along those lines) somewhere?
^Doesn't seem that way to me. Even in compound #1 (alpha-ethyl mescaline) he has this whimsical passage (red text shows references to past events):
The implication is that 3,4,5-trimethoxyamphetamine (TMA, #157) had already been synthesized and assayed, was found to be twice as potent as mescaline, and Shulgin then set out to test whether longer alpha-alkyl extensions would show a continual escalation in potency. In this vein he synthesized and assayed AEM.
Plus, from an administrative standpoint, common families have common precursors (obviously ordered in bulk), and some of these have poor shelf lives. Why place yourself in a position in which you have to continually discard and reorder precursors when you can utilize economies of scale to streamline your budget?
The implication is that 3,4,5-trimethoxyamphetamine (TMA, #157) had already been synthesized and assayed, was found to be twice as potent as mescaline, and Shulgin then set out to test whether longer alpha-alkyl extensions would show a continual escalation in potency. In this vein he synthesized and assayed AEM.
Plus, from an administrative standpoint, common families have common precursors (obviously ordered in bulk), and some of these have poor shelf lives. Why place yourself in a position in which you have to continually discard and reorder precursors when you can utilize economies of scale to streamline your budget?
nuke
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As many of the items in PiHKAL were synthesized in part and then shelved and returned to later, it's difficult to get a chronology for the compounds. The same thing goes for the bioassays. The closest thing you'll get to chronological order would be the stuff in the first books of PiHKAL/TiHKAL.
You can also go through Shulgin's list of publications to see when he published about various compounds.
You can also go through Shulgin's list of publications to see when he published about various compounds.
x89
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Perhaps an easy one: Where's a good place for one with mediocre knowledge of chemistry but 168 hours a week of free time and a burning desire for knowledge to self teach this stuff. Are there any areas which are easier to start on? I believe the encompassing subject is called "Organic Chemistry" am I right?!
Computing is my area of expertise but that's a dawdle!
Computing is my area of expertise but that's a dawdle!
Anyone looking to hone their OChem skills I found this page to be rather useful.
http://evans.harvard.edu/problems/index.cgi
http://evans.harvard.edu/problems/index.cgi
DavisK4high247
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I cannot find any info on any websites on this medicine I got for nasal use after a surgery 2 days ago( cocaine and neosynephrine nasal drops ) can anyone help me find the chemical makeup of these drops and in what amount of each drug is prsent in this soulution and maybe the ph of the solution,it says saline cocaine drops with noesynephrine and it stops the bleeding and somwhat dums the stiched up area but does not seem to absorb into the bloodstop nasaly or through the stitced area which are still fresh and should absorb any cocaine into the bloodstram unless it is ph designed or something to be non soluble internasaly to absorb more that at a very small localized are? any help would be appreciated and as quicky as possible as well would be of great help.Thank You
phase_dancer
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It describes substitution on a Nitrogen....e.g. N-methyl-1-phenyl-propan-2-amine (methamphetamine); N,N-dimethyl-1-phenylpropan-2-amine (dimethylamphetamine)
brown sugar
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hello im new here
Astavats
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Pharmacokinetics
I'd like to learn more about metabolization of various drugs, how certain groups may or may not get removed/replaced, and so forth. Does anyone have suggestions where I could begin? Websites, books, texts, videos, anything would be appreciated, especially if it's publicly available.
It's fine if it's ahead of me, I have no exceptions of digesting all the information at once.
All the best.
I'd like to learn more about metabolization of various drugs, how certain groups may or may not get removed/replaced, and so forth. Does anyone have suggestions where I could begin? Websites, books, texts, videos, anything would be appreciated, especially if it's publicly available.
It's fine if it's ahead of me, I have no exceptions of digesting all the information at once.
All the best.
phase_dancer
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A basic pharmacology text is a good place to start
I found Rang et al "Pharmacology" a fairly good text.
It's also worth getting an metabolic pathways wall chart. Sigma Aldrich used to have a good free chart.
Here's a few that have been available online as e-books
Drug Metabolism Current Concepts Edited by Corina Ionescu and Mino R. Caira
Pharmacokinetics and Metabolism in Drug Design
Edited by D. A. Smith, H. van de Waterbeemd, D. K. Walker, R. Mannhold, H. Kubinyi, H.Timmerman
If you're feeling like getting in up to your ears
Comprehensive Enzyme Kinetics by Vladimir Leskovac
I found Rang et al "Pharmacology" a fairly good text.
It's also worth getting an metabolic pathways wall chart. Sigma Aldrich used to have a good free chart.
Here's a few that have been available online as e-books
Drug Metabolism Current Concepts Edited by Corina Ionescu and Mino R. Caira
Pharmacokinetics and Metabolism in Drug Design
Edited by D. A. Smith, H. van de Waterbeemd, D. K. Walker, R. Mannhold, H. Kubinyi, H.Timmerman
If you're feeling like getting in up to your ears
Comprehensive Enzyme Kinetics by Vladimir Leskovac
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