Advertisement
Chromatography Forum

thienopyridines

Discussions about HPLC, CE, TLC, SFC, and other "liquid phase" separation techniques.

5 posts Page 1 of 1
Post a reply

thienopyridines

avatar
Ivo
Hi to everyone

I am working on thienopyridine class of substance and have some problem with selectivity of two. I am using C18 100x2.1, 1,8 um but I am wondering is there any better choice for thienopyridines... I was thinking of Phenyl-Hexyl or Fluoro-Phenyl phase column. Any suggestions?

Thanks
Regards,
Ivan

Re: thienopyridines

avatar
schlepro
Dear Ivan,

Without a little more information, all I can say is check the column catalogs/lit. The structures look like something that could run just fine on a C18, and you'll probably need acid (e.g. 0.1% TFA) in your aqueous channel in order to get Prasugrel to resolve. My experience is that there is nothing sacred about ones stationary phase, so I doubt you will gain much from using a phenyl-hexyl column or similar. Can you provide more about your run conditions (H/U plc, mobile phase, gradient, temperature, flow)? Which compounds are coeluting? Do you need the method to work with, say Cysteine as well?

Sincerely,
Keith

Re: thienopyridines

avatar
Ivo
Dear Keith,

Thank you very much for replay. I was out of lab over holidays so I reposted with some delay... btw, have a successful new year... with lots of fun, of course ;)

I am working on Ticlopidine, 5-(2-Chlorobenzyl)-4,5,6,7-tetrahydrothienol[3,2-c]pyridine. It nearly coelut with similar impuriti.. only difference is sulfur position in thienopyridine ring (---tetrahydrothienol[2,3-c]pyridine). Second imp. wich I would like to separate more is N-(2-chlorobenzyl)-2-(thiophen-2-yl)ethanamine (basically ticlopidine with open N-ring). Run conditions are: UPLC; mob A (Na-pentansulfonate, monohydrate buffer), ph 3.4 with H3PO4; mob B (100% MeOH); gradient (initial 30%A-70%B, 10 min 70%A-30%B, 11 min 30%A-70%B, 13 min 30%A-70%B); flow 0.5 ml/min; temp: 45 cels/deg; 220 nm.
I have tried different mobile phases and gradients and I find this most satisfactory, though, I will appreciate any comments regarding those conditions or any other. I was thinking about phenyl columns because all analytes contains some kind of ring and according to catalogs have some advance over C18.

Sincerely,
Ivan

Re: thienopyridines

avatar
Vlad Orlovsky
Since all your compounds are ionic and hydrophobic, your best bet for separation is mixed-mode. Here is how mixed-mode can be used for separation of isomers:
http://www.sielc.com/Compound-O-Toluidine.html
http://www.sielc.com/Compound-4-Aminosa ... -Acid.html
http://www.sielc.com/Compound-3-5-Dihyd ... -Acid.html

Contact me if you have questions.
Vlad Orlovsky
HELIX Chromatography
My opinions might be bias, but I have about 1000 examples to support them. Check our website for new science and applications
www.helixchrom.com

Re: thienopyridines

avatar
Ivo
Vlad, thank you very much for replay and info.
I´d feel free to contact you for more questions.

Sincerely,
Ivan
Post a reply
5 posts Page 1 of 1
Return to “Liquid Chromatography”

Who is online

In total there are 19 users online :: 4 registered, 0 hidden and 15 guests (based on users active over the past 5 minutes)
Most users ever online was 4374 on Fri Oct 03, 2025 12:41 am
Users browsing this forum: Amazon [Bot], Baidu [Spider], Bing [Bot], Google [Bot] and 15 guests

Latest Blog Posts from Separation Science

Separation Science offers free learning from the experts covering methods, applications, webinars, eSeminars, videos, tutorials for users of liquid chromatography, gas chromatography, mass spectrometry, sample preparation and related analytical techniques.

Subscribe to our eNewsletter with daily, weekly or monthly updates: Food & Beverage, Environmental, (Bio)Pharmaceutical, Bioclinical, Liquid Chromatography, Gas Chromatography and Mass Spectrometry.

Liquid Chromatography

    Gas Chromatography

      Mass Spectrometry