OpenSourceMalaria:Story so far: Difference between revisions

From OpenWetWare
Jump to navigationJump to search
(First major injection of words)
(31 intermediate revisions by 3 users not shown)
Line 1: Line 1:
{{OSDDMalaria}}
{{OSDDMalaria}}


''This is a human-readable summary of the first open source drug discovery for malaria project. A less readable collection of all the relevant data can be found [[OSDDMalaria:GSK_Arylpyrrole_Series|here]].''
''This is a human-readable summary of the open source drug discovery for malaria project. A less readable collection of all the relevant data can be found [[OSDDMalaria:GSK_Arylpyrrole_Series|here]].''
 
'''Note: This page is currently (May 2 2012) being built, so some links are missing.'''


=The story so far in the open source drug discovery for malaria project=
=The story so far in the open source drug discovery for malaria project=
Line 9: Line 7:
==History==
==History==


Last year my lab received seed funding for a pilot project in open source drug discovery from the Medicines for Malaria Venture. Our project champion at the outset was Tim Wells, who had clearly been thinking along similar lines to me - rather than debate the idea of open source drug discovery any more, let's just try it. Jeremy Burrows quickly came on board and led the suggestion to go after a few of the actives that had been placed in the public domain in 2010 by GlaxoSmithKline. We got started in the lab in August 2011. We were successful in securing further funding from an ARC Linkage grant - a scheme where funds from an external agency are matched by the Australian Government. This has given us funding from May 2012 for three years - so we have enough money to drive this project for the moment to see if it works.
Last year [http://openwetware.org/wiki/Todd the Todd lab] at The University of Sydney received funding for a pilot project in open source drug discovery from the Medicines for Malaria Venture (MMV). The project champion at the outset was [http://www.mmv.org/about-us/our-team/tim-wells Tim Wells]. [http://www.mmv.org/about-us/our-team/jeremy-burrows Jeremy Burrows] came on board and led the suggestion to go after a few of the actives that had been [http://www.nature.com/nature/journal/v465/n7296/abs/nature09107.html placed in the public domain in 2010] by GlaxoSmithKline and others. Work got [http://malaria.ourexperiment.org/tcmdc_ap/1/PaalKnorr_Synthesis_of_1aryl25dimethyl_Pyrrole_Core_PMY_11.html underway in the lab] in August 2011. The team were [http://sydney.edu.au/research_support/funding/arc/linkage_2012.shtml successful] in securing further funding from an Australian Research Council Linkage grant - a scheme where funds from an external agency are matched by the Australian Government. This has generated funding from May 2012 for three years.
 
The scientific idea behind the project is familiar medicinal chemistry methodology - the aim is to find a small molecule that is effective for the treatment of malaria, and that involves generating molecules (the Todd lab's primary responsibility) and evaluating them (with other members of the project). Based on the biological results, analogs are made, or the series might be ditched and another one selected. The first series to be tried is based on an [http://openwetware.org/wiki/OSDDMalaria:GSK_Arylpyrrole_Series arylpyrrole] that was one of the most attractive hits in the [https://www.ebi.ac.uk/chemblntd/#tcams_dataset original GSK dataset], but there are [http://pubs.acs.org/doi/abs/10.1021/ml200135p plenty of other series that are also very attractive] from a medchem perspective.
 
The difference with this project though (as described in the [http://www.thesynapticleap.org/node/343 6 Laws]) is that everything is open, meaning all the experiments go on the web (including the ones that did not turn out well). All the data are available. Anyone can do anything they wish with the compounds, with the proviso the project is cited (see licence conditions below). The main difference is that anyone can take part - people may make molecules, offer guidance and input in other ways that ''change the direction of the project as it is happening'', i.e. rather than the release of all data at the end of the project, data are released as the project is happening so that people can become genuinely involved in the research. Thus the iterative cycle of analog synthesis in response to biological data that is normally guided by luck and medchem intuition is now guided by the intuition of the collective. Similarly, since the biological data are all open too, it should be easier to form an objective assessment of a molecule's performance divorced from the judgement of those closest to the compounds. In the same way that in software development "[http://en.wikipedia.org/wiki/Linus%27_Law with enough eyeballs all bugs are shallow]" the open nature of the research makes the science better and faster. This was found to be the case in a [http://www.nature.com/nchem/journal/v3/n10/full/nchem.1149.html previous synthetic chemistry project involving the drug praziquantel].


Naturally we're all really excited about this. The scientific idea behind the project is familiar medicinal chemistry territory - we need to find a small molecule that is effective for the treatment of malaria, and we will do that by making molecules (my lab's primary responsibility) and evaluating them (with collaborators). Based on those results, we make analogs, or ditch the series and pick another. We started with the arylpyrrole series that was one of the most attractive sets in the original GSK dataset, but there are plenty of others that are also very attractive from a medchem perspective.
==Three Rounds of Synthesis and Evaluation==


The difference with this project though (as we previously described in the 6 Laws) is that everything is open, meaning all the experiments go on the web (including the ones that did not turn out well). All the data are available. Anyone can do anything they wish with the compounds, with the proviso we are cited - the licence for the project is CC-BY-3.0, though this is sometimes not yet clear on all the various websites we use. The main difference is that anyone can take part - that people may make molecules, offer guidance and input in other ways that change the direction of the project as it is happening. i.e. rather than releasing all our data at the end of the project we release as the project is happening so that people can really become involved in the research. Thus the iterative cycle of analog synthesis in response to biological data that is normally guided by a kind of medchem intuition is now guided by the intuition of the collective. Similarly, since the biological data are all open too, it should be easier to form an objective assessment of a molecule's performance divorced from the judgement of those closest to the compounds. In the same way that in software development "with enough eyeballs all bugs are shallow" we hope that the open nature of the research makes the science better and faster. As it did with our previous synthetic project with praziquantel.
[https://plus.google.com/u/0/b/114702323662314783325/115627447826173336765/posts Paul Ylioja] started by resynthesising the two known active compounds from the GSK set (OSM-S-5 and OSM-S-6), plus a few simple derivatives, and [http://www.thesynapticleap.org/node/367 confirming that they were active]. The current list of all the compounds made thus far in this part of the project is kept in [http://bit.ly/OSDDcompounds this spreadsheet]. The [http://malaria.ourexperiment.org/biological_data/month/1325376000 biological evaluation] was carried out by three separate labs ([http://www.discoverybiology.org/team/vicky-avery Vicky Avery], [http://www.bio21.org/group-leaders/bio-chemistry/stuart-ralph Stuart Ralph] and the [http://www.gsk.com/collaborations/tres-cantos.htm original GSK Tres Cantos Lab led by Javier Gamo]) to ensure a solid footing of repeatability. The original compounds contained an ester which was thought likely to hydrolyze ''in vivo'', so various versions of the "lower half" of these leads were also evaluated to check whether the original hits were prodrugs, but all these compounds were found to be inactive. The project champion from MMV, [http://www.mmv.org/about-us/our-team/paul-willis Paul Willis], [http://www.thesynapticleap.org/node/349 recommended] a few "near neighbor" compounds that also looked interesting, and a number of these were made too and evaluated in this first round. One compound, OSM-S-9, was found to be more active than the original GSK hits. [https://plus.google.com/u/0/111817031902595048944/posts Sanjay Batra] came on board the project and his student [https://plus.google.com/u/0/113151089809892205923/posts Soumya] made (and is making)[http://malaria.ourexperiment.org/cdriarylpyrroles some analogs] varying in the position of the fluorine atom, though the activity of those tested to date is low. (Sanjay works at the [http://www.cdriindia.org/analytical.htm CDRI] in Lucknow, India, where [https://plus.google.com/u/0/116616719379353298385/posts Saman Habib] also works - Saman is leading the [http://malaria.osdd.net/ Indian OSDDm project] which will hopefully get started soon). The outcome was that the original hits remained interesting (because of their reasonable potency and logP values) but that highly potent novel antimalarials were also being generated in this class. Thus a [http://www.thesynapticleap.org/node/381 second set of compounds was synthesized and evaluated], giving rise to several new highly potent compounds, one of which (OSM-S-39) displayed a picomolar IC50 value. This is impressive given the small number of compounds made to date, and is testament to the quality of the hits contained in the original GSK set.


==Early Stages of the Project==
[[Image:Compounds of Interest in Update.png|thumb|center|500px| '''Original and Representative Potent Compounds in the Arylpyrrole Series]]


Paul Ylioja started by resynthesising the two known active compounds from the GSK set, plus a few simple derivatives, and confirming that they were active. The biological evaluation was carried out by three separate labs to ensure we were on a solid footing. Our MMV project champion Paul Willis recommended a few "near neighbor" compounds that also looked interesting, and we made a number of these too, which were again evaluated. Sanjay Batra came on board the project and his student Soumya made some analogs that will be included in our first paper, though their activity is low. Sanjay works at the CDRI in Lucknow, India, where Saman Habib also works - Saman is leading the Indian OSDDm project which will shortly get started. The outcome was that the original hits remained interesting (because of their reasonable potency and logP values) but that we were clearly also generating highly potent novel antimalarials in this class. One compound was coming out picomolar. This is quite impressive given the small number of compounds made to date, and is perhaps testament to the quality of the hits contained in the GSK set.
At this point the decision was taken to take the most promising compounds on to advanced biological evaluation, to see what the promise of this class really is (rather than continue to increase potency through analog synthesis). Evaluations to date are as follows.


Several compounds have been sent for metabolism assays to Sue Charman's lab at Monash and we are waiting for the results. The two original GSK compounds as well as the highly potent near neighbor X are currently being evaluated in mice. Compound X and Y were recently subjected to the hERG assay and passed, implying that they should not exhibit cardiac side effects. Several of the compounds have also been evaluated in a gametocyte assay with interesting results that may suggest they have activity in blocking the transmission of the parasite.
* '''Metabolic and solubility assays''': The two original GSK compounds and six other compounds made in this project were evaluated by [http://www.pharm.monash.edu.au/staff/sacharman.html Sue Charman's lab at Monash]. The raw data are [http://malaria.ourexperiment.org/biological_data/3101 here] and can be discussed [http://www.thesynapticleap.org/node/401 here]. The originals displayed good solubility but moderate degradation rates. The other compounds were degraded more slowly but at a cost of low solubility.
* '''hERG''': One of the original GSK compounds (OSM-S-5) plus one of the most potent novel compounds identified to date (OSM-S-35) were subjected to the [http://malaria.ourexperiment.org/biological_data/2999 hERG assay and passed], perhaps implying that this class of compounds should not exhibit undesirable cardiac side effects. Discussion page [http://www.thesynapticleap.org/node/402 here].
* '''Late Stage Gametocyte Assay''': Four of the compounds have also been [http://malaria.ourexperiment.org/biological_data/3066 evaluated in a late stage gametocyte assay] with very interesting results indicating unusually high activity in blocking the transmission of the parasite. The original GSK compound OSM-S-5 was inactive. Discussion page [http://www.thesynapticleap.org/node/403 here].
* '''In vivo''': However, the two original GSK compounds as well as one of the most promising novel compounds have been evaluated in mice and found to possess zero oral efficacy (Results available [http://malaria.ourexperiment.org/uri/ed here]). This result taken with all the other biological data requires careful consideration about whether to change the focus of the research to another series or whether to continue to alter the structures of the best compounds to overcome the ''in vivo'' roadblock.
 
Based on these results it was decided to carry out a third round of analog synthesis and evaluation on the arylpyrrole series, with an emphasis on analogs a) with low logP and b) that lack the thiazolidinone heterocycle. A consultation [http://www.thesynapticleap.org/node/412 occurred] asking for suggestions for the ten most appropriate compounds to make, and the 10 most interesting for commercial procurement. The final stage of the consultation took place [http://www.youtube.com/watch?v=ooM8kuo14Bg live on the web]. As a result the lists were [http://www.thesynapticleap.org/node/416 finalised] and the compounds need to be ordered and made. Currently (Sept 2012) there remain a few compounds which need synthetic input from any labs interested in contributing. The project has to date had no luck in securing donations of the compounds from commercial suppliers.


==What Are the Compounds Doing?==
==What Are the Compounds Doing?==


What might these compounds be doing? We're not sure. The original screens were whole-cell assays, so while we know they're effective, we don't know what they're doing. Iain Wallace from ChEMBL has done a very neat prediction of these compounds (as well as predictions for the whole malaria box, which is a set of compounds MMV are providing to people for antimalarial screening and which are the focus of a current round of Gates requests for proposals). Iain's able to cluster compounds as a similarity map, which is a neat way of visualizing the correlation between structure and predicted activity. Are these predictions right? We're seeking to examine that by sending a subset of compounds to Corey Nislow at the University of Toronto for examination in a yeast-based assay he's developed.
What might this series of compounds be doing to the parasite to kill it so effectively? It's not clear. The original screens were whole-cell assays, so while it is known that the compounds are effective, it's not known what they are doing in any detail. Iain Wallace from ChEMBL has performed [http://www.thesynapticleap.org/node/387 a prediction] of the biological role of these compounds (as well as predictions for the whole "[http://www.mmv.org/malariabox Malaria Box]", which is a set of compounds MMV are providing to people for antimalarial screening and which are the focus of a [http://www.grandchallenges.org/Explorations/Topics/Pages/AntimalarialCompoundsRound9.aspx current round] of Gates requests for proposals). Iain clustered the compounds as a similarity map, allowing visualization of the correlation between structure and predicted activity. Discussed also [https://plus.google.com/u/0/b/114702323662314783325/114702323662314783325/posts/F5B9nA2sJLr here]. One of the predictions was that the compounds hit an enzyme known as DHODH, and GSK are at the time of writing screening some of the project's compounds against this enzyme. These predictions are made using informatics - a comparison of the structures of our compounds with other known compounds that have known activities. The argument is based on extrapolation. To evaluate whether the prediction is correct, a subset of compounds has been sent to [http://chemogenomics.med.utoronto.ca/hiplab/index.php Corey Nislow] at the University of Toronto for screening in a yeast-based assay that does not identify for sure what the compounds are doing (which is very difficult) but provides harder biological evidence for a role.


==How do we Obtain Other Compounds?==
==How to Obtain Other Compounds==


The original compounds from the GSK assay were commercially-available. Rather than make compounds that might be sourced by other means, what about obtaining commercially-available compounds of interest from the suppliers, either through purchase or donation? Iain again came to help us with this by finding commercially-available compounds through an emolecules search which looked similar to those we are interested in (actually for a related series, see below). Now we have to see whether we can actually obtain these compounds. It's an interesting conundrum - we know that there are compounds sitting in fridges that are related to our most active antimalarials, and all we need are a few milligrams. How do we get hold of these most efficiently? And what about compounds that are not commercially-available? Are there compounds in academic labs that we could evaluate, such as those from the Roberts lab at Scripps (whom we've contacted). What about compounds that are unpublished, but may be excellent candidates for screening? It would be useful to have a needs-driven marketplace for molecules, like a Molecular Craigslist, but it doesn't really exist.
The original compounds from the GSK assay were commercially available, arising from libraries that are provided to larger companies by smaller specialised companies. In a medicinal chemistry project like this one starts with a set of compounds, then one sources further compounds that are similar. Novel compounds need to be made. Other compounds may be available by other means, however. Typically in academia required compounds are made in-house because academia works as a closed system, which is inefficient if relevant compounds exist elsewhere on the planet and can be sourced by other means more quickly. In this project organic synthesis of ''novel compounds'' is currently being performed in Sydney and Lucknow. But for ''known'' compounds the following needs to be done.


==Related Series==
1) '''Identification of Commercial Compounds:''' What if some compounds we require are already commercially available? How can these be found? Iain Wallace [http://www.thesynapticleap.org/node/399 was able to do a search] of databases such as eMolecules for relevant compounds above a certain threshold of similarity and filter compounds by supplier, generating the "hitlist" quickly and with no manual human input. These can be converted into spreadhseets for quick visualisation - see [https://plus.google.com/u/0/b/114702323662314783325/115975655197247500095/posts/X2Djh2szx9F here] for examples on Jimmy Cronshaw's series (see below for these).
 
2) '''Obtaining Commercial Compounds:''' With the compounds identified, the relevant suppliers need to be contacted to ask for donations. That will probably not be trivial since it needs a human interaction. Failing that the compounds can just be bought.


In parallel an Honours student in the lab, Jimmy Cronshaw, has started the synthesis of two other hits from the GSK set, again to confirm activity. He's nearly finished one, and is about to do the difficult part of the other series. Again, these are very attractive hits to be pursuing.
3) '''Identification of Other/academic Compounds:''' What about compounds that could be useful to the project but which are not commercially available, e.g. compounds sitting in academic lab fridges? Some can be found using resources like SciFinder, though these require expensive subscriptions. Many compounds that might be perfect for the project may not even be in the published literature, which is another argument for openness in science.


==Open Source Drug Discovery More Generally==
4) '''Get Other/academic Compounds:''' This will be a case of manual contact with interested groups. [https://plus.google.com/u/0/b/114702323662314783325/114702323662314783325/posts/VmPupxxrWEr One such enquiry] has already been submitted, to see what happens. Naturally contributions are rewarded by possible authorship on resulting papers.


We held an interesting one-day meeting on open source drug discovery for malaria where we discussed general issues surrounding open drug discovery, followed by more specific malaria-related ideas. These talks are gradually going up on YouTube, and they frame many of the issues very well, for example the landscape of drug discovery in neglected diseases, and whether patents are necessary in drug discovery. More coming as and when we can do the annotation properly.
Ultimately, as a species, we are not very efficient at sharing valuable chemical resources. A user-driven list would be helpful - "I need compound X. I can buy it from you, or you can give it to me, or you can make it for me or with me, but I need the compound in timeframe Y." This is like a [http://intermolecular.wordpress.com/2012/04/20/molecular-craigslist/ Molecular Craigslist], and would reduce some of the supply-demand barriers in chemical research.


==How We Run the Project==
==Related Series==


The technical background to the project is also interesting, though as with everything in this project we're open to suggestions. We're using Labtrove for recording the raw data in electronic lab notebooks. We're using this site to coordinate and discuss ideas. We're increasingly using Google+ for discussion of small points, and Twitter as a broadcast mechanism for updates. We have not used LinkedIn as much as we did for the praziquantel project. We employ a wiki to host the current description of where the project is at. These sites are all quite intuitive and simple, but all have their limitations.  
The arypyrrole series is the first to be examined. A forked series, the [http://openwetware.org/wiki/OSDDMalaria:Arylpyrazole_Series pyrazoles], looks attractive but has not yet received a great deal of input. Two other interesting-looking starting points from the GSK set, based on a [http://openwetware.org/wiki/OSDDMalaria:GSK_Triazolourea_Singleton triazolourea] and a [http://openwetware.org/wiki/OSDDMalaria:GSK_Amino-thienopyrimidine_Series thienopyrimidine], are currently being resynthesised by [https://plus.google.com/u/0/b/114702323662314783325/115975655197247500095/posts James Cronshaw] in Sydney to confirm their activity, upon which time it will be necessary to decide which, if either, are to be taken on further. In general a strategy for the project is to decide as early as possible which series are looking attractive biologically, because there are still a lot of leads to pursue. If any of these structures look synthetically attractive to you based on your previous experience, please consider joining the project. Some of these molecules are quite straightforward to make and would be suitable for undergraduate lab classes.


==Why Take Part?==
==Comments==


What of motivations? Why would people contribute? Partly to solve a problem. Partly to be involved with quality science that is open, and hence subject to the most brutal form of ongoing peer-review. Partly for academic credentials (since we'll soon be publishing a paper). Partly to demonstrate competence. Perhaps a mixture of all these things.
Comments and input can be by [http://twitter.com/#!/osddmalaria Twitter], [https://plus.google.com/u/0/b/114702323662314783325/114702323662314783325/posts Google+], [http://www.thesynapticleap.org/node/342 The Synaptic Leap] or directly on the relevant [http://malaria.ourexperiment.org/ Electronic Lab Notebooks]. This page also has a "talk" tab for input. Or please write your own input somewhere (''e.g.'', your own blog) and link to the project. Anonymity is perfectly acceptable, just less useful. Please avoid email.


We're playing with the idea of a competition, though - or rather a prize. While we have certainly led the way to a very promising lead compound, we are acutely aware that there is a long road towards having a compound look sufficiently promising that it moves towards clinical trials. There's a lot of tweaking, and perhaps even the move to another series. Who knows. It's likely we will need a lot more input that we have currently been getting, and so we're playing with whether to launch a prize to stimulate input. It would be a teamless prize, awarded based on performance of individuals within a group where everything is shared. Difficult to judge, difficult to award, and hence worth doing.
==Licence==


A final point - the project is open. We don't own it. It exists in itself and those people most active in the project lead it. If you wish to contribute, in any capacity, please do so. There is no need to "clear" anything with me by email first. It's often the case that I will receive questions/suggestions by email. In the development of Linux, the need for Linus to approve everything caused problems, and the observation that "Linus doesn't scale". Well I don't scale either, so it's more efficient if all our discussions are held publicly. I know that a lot of people don't like this. In science we don't tend to get the idea of "beta testing" something. When data are released in science there is an expectation that the data are correct, and usually accompanied by an explanation. I don't understand this view. I'm comfortable with release of data immediately, and then I'm happy to apply a caution filter that makes me skeptical of things until repeated, or makes me unsurprised when a repeat fails.
The project's licence unless otherwise stated is [http://creativecommons.org/licenses/by/3.0/ CC-BY-3.0] meaning you can use whatever you want for whatever purpose, provided you cite the project.

Revision as of 21:37, 31 October 2012

Malaria Home        OSM So Far        Compound Series        Links        Open Source Research Home        Tech Ops        FAQ       


This is a human-readable summary of the open source drug discovery for malaria project. A less readable collection of all the relevant data can be found here.

The story so far in the open source drug discovery for malaria project

History

Last year the Todd lab at The University of Sydney received funding for a pilot project in open source drug discovery from the Medicines for Malaria Venture (MMV). The project champion at the outset was Tim Wells. Jeremy Burrows came on board and led the suggestion to go after a few of the actives that had been placed in the public domain in 2010 by GlaxoSmithKline and others. Work got underway in the lab in August 2011. The team were successful in securing further funding from an Australian Research Council Linkage grant - a scheme where funds from an external agency are matched by the Australian Government. This has generated funding from May 2012 for three years.

The scientific idea behind the project is familiar medicinal chemistry methodology - the aim is to find a small molecule that is effective for the treatment of malaria, and that involves generating molecules (the Todd lab's primary responsibility) and evaluating them (with other members of the project). Based on the biological results, analogs are made, or the series might be ditched and another one selected. The first series to be tried is based on an arylpyrrole that was one of the most attractive hits in the original GSK dataset, but there are plenty of other series that are also very attractive from a medchem perspective.

The difference with this project though (as described in the 6 Laws) is that everything is open, meaning all the experiments go on the web (including the ones that did not turn out well). All the data are available. Anyone can do anything they wish with the compounds, with the proviso the project is cited (see licence conditions below). The main difference is that anyone can take part - people may make molecules, offer guidance and input in other ways that change the direction of the project as it is happening, i.e. rather than the release of all data at the end of the project, data are released as the project is happening so that people can become genuinely involved in the research. Thus the iterative cycle of analog synthesis in response to biological data that is normally guided by luck and medchem intuition is now guided by the intuition of the collective. Similarly, since the biological data are all open too, it should be easier to form an objective assessment of a molecule's performance divorced from the judgement of those closest to the compounds. In the same way that in software development "with enough eyeballs all bugs are shallow" the open nature of the research makes the science better and faster. This was found to be the case in a previous synthetic chemistry project involving the drug praziquantel.

Three Rounds of Synthesis and Evaluation

Paul Ylioja started by resynthesising the two known active compounds from the GSK set (OSM-S-5 and OSM-S-6), plus a few simple derivatives, and confirming that they were active. The current list of all the compounds made thus far in this part of the project is kept in this spreadsheet. The biological evaluation was carried out by three separate labs (Vicky Avery, Stuart Ralph and the original GSK Tres Cantos Lab led by Javier Gamo) to ensure a solid footing of repeatability. The original compounds contained an ester which was thought likely to hydrolyze in vivo, so various versions of the "lower half" of these leads were also evaluated to check whether the original hits were prodrugs, but all these compounds were found to be inactive. The project champion from MMV, Paul Willis, recommended a few "near neighbor" compounds that also looked interesting, and a number of these were made too and evaluated in this first round. One compound, OSM-S-9, was found to be more active than the original GSK hits. Sanjay Batra came on board the project and his student Soumya made (and is making)some analogs varying in the position of the fluorine atom, though the activity of those tested to date is low. (Sanjay works at the CDRI in Lucknow, India, where Saman Habib also works - Saman is leading the Indian OSDDm project which will hopefully get started soon). The outcome was that the original hits remained interesting (because of their reasonable potency and logP values) but that highly potent novel antimalarials were also being generated in this class. Thus a second set of compounds was synthesized and evaluated, giving rise to several new highly potent compounds, one of which (OSM-S-39) displayed a picomolar IC50 value. This is impressive given the small number of compounds made to date, and is testament to the quality of the hits contained in the original GSK set.

Original and Representative Potent Compounds in the Arylpyrrole Series

At this point the decision was taken to take the most promising compounds on to advanced biological evaluation, to see what the promise of this class really is (rather than continue to increase potency through analog synthesis). Evaluations to date are as follows.

  • Metabolic and solubility assays: The two original GSK compounds and six other compounds made in this project were evaluated by Sue Charman's lab at Monash. The raw data are here and can be discussed here. The originals displayed good solubility but moderate degradation rates. The other compounds were degraded more slowly but at a cost of low solubility.
  • hERG: One of the original GSK compounds (OSM-S-5) plus one of the most potent novel compounds identified to date (OSM-S-35) were subjected to the hERG assay and passed, perhaps implying that this class of compounds should not exhibit undesirable cardiac side effects. Discussion page here.
  • Late Stage Gametocyte Assay: Four of the compounds have also been evaluated in a late stage gametocyte assay with very interesting results indicating unusually high activity in blocking the transmission of the parasite. The original GSK compound OSM-S-5 was inactive. Discussion page here.
  • In vivo: However, the two original GSK compounds as well as one of the most promising novel compounds have been evaluated in mice and found to possess zero oral efficacy (Results available here). This result taken with all the other biological data requires careful consideration about whether to change the focus of the research to another series or whether to continue to alter the structures of the best compounds to overcome the in vivo roadblock.

Based on these results it was decided to carry out a third round of analog synthesis and evaluation on the arylpyrrole series, with an emphasis on analogs a) with low logP and b) that lack the thiazolidinone heterocycle. A consultation occurred asking for suggestions for the ten most appropriate compounds to make, and the 10 most interesting for commercial procurement. The final stage of the consultation took place live on the web. As a result the lists were finalised and the compounds need to be ordered and made. Currently (Sept 2012) there remain a few compounds which need synthetic input from any labs interested in contributing. The project has to date had no luck in securing donations of the compounds from commercial suppliers.

What Are the Compounds Doing?

What might this series of compounds be doing to the parasite to kill it so effectively? It's not clear. The original screens were whole-cell assays, so while it is known that the compounds are effective, it's not known what they are doing in any detail. Iain Wallace from ChEMBL has performed a prediction of the biological role of these compounds (as well as predictions for the whole "Malaria Box", which is a set of compounds MMV are providing to people for antimalarial screening and which are the focus of a current round of Gates requests for proposals). Iain clustered the compounds as a similarity map, allowing visualization of the correlation between structure and predicted activity. Discussed also here. One of the predictions was that the compounds hit an enzyme known as DHODH, and GSK are at the time of writing screening some of the project's compounds against this enzyme. These predictions are made using informatics - a comparison of the structures of our compounds with other known compounds that have known activities. The argument is based on extrapolation. To evaluate whether the prediction is correct, a subset of compounds has been sent to Corey Nislow at the University of Toronto for screening in a yeast-based assay that does not identify for sure what the compounds are doing (which is very difficult) but provides harder biological evidence for a role.

How to Obtain Other Compounds

The original compounds from the GSK assay were commercially available, arising from libraries that are provided to larger companies by smaller specialised companies. In a medicinal chemistry project like this one starts with a set of compounds, then one sources further compounds that are similar. Novel compounds need to be made. Other compounds may be available by other means, however. Typically in academia required compounds are made in-house because academia works as a closed system, which is inefficient if relevant compounds exist elsewhere on the planet and can be sourced by other means more quickly. In this project organic synthesis of novel compounds is currently being performed in Sydney and Lucknow. But for known compounds the following needs to be done.

1) Identification of Commercial Compounds: What if some compounds we require are already commercially available? How can these be found? Iain Wallace was able to do a search of databases such as eMolecules for relevant compounds above a certain threshold of similarity and filter compounds by supplier, generating the "hitlist" quickly and with no manual human input. These can be converted into spreadhseets for quick visualisation - see here for examples on Jimmy Cronshaw's series (see below for these).

2) Obtaining Commercial Compounds: With the compounds identified, the relevant suppliers need to be contacted to ask for donations. That will probably not be trivial since it needs a human interaction. Failing that the compounds can just be bought.

3) Identification of Other/academic Compounds: What about compounds that could be useful to the project but which are not commercially available, e.g. compounds sitting in academic lab fridges? Some can be found using resources like SciFinder, though these require expensive subscriptions. Many compounds that might be perfect for the project may not even be in the published literature, which is another argument for openness in science.

4) Get Other/academic Compounds: This will be a case of manual contact with interested groups. One such enquiry has already been submitted, to see what happens. Naturally contributions are rewarded by possible authorship on resulting papers.

Ultimately, as a species, we are not very efficient at sharing valuable chemical resources. A user-driven list would be helpful - "I need compound X. I can buy it from you, or you can give it to me, or you can make it for me or with me, but I need the compound in timeframe Y." This is like a Molecular Craigslist, and would reduce some of the supply-demand barriers in chemical research.

Related Series

The arypyrrole series is the first to be examined. A forked series, the pyrazoles, looks attractive but has not yet received a great deal of input. Two other interesting-looking starting points from the GSK set, based on a triazolourea and a thienopyrimidine, are currently being resynthesised by James Cronshaw in Sydney to confirm their activity, upon which time it will be necessary to decide which, if either, are to be taken on further. In general a strategy for the project is to decide as early as possible which series are looking attractive biologically, because there are still a lot of leads to pursue. If any of these structures look synthetically attractive to you based on your previous experience, please consider joining the project. Some of these molecules are quite straightforward to make and would be suitable for undergraduate lab classes.

Comments

Comments and input can be by Twitter, Google+, The Synaptic Leap or directly on the relevant Electronic Lab Notebooks. This page also has a "talk" tab for input. Or please write your own input somewhere (e.g., your own blog) and link to the project. Anonymity is perfectly acceptable, just less useful. Please avoid email.

Licence

The project's licence unless otherwise stated is CC-BY-3.0 meaning you can use whatever you want for whatever purpose, provided you cite the project.

Retrieved from "https://openwetware.org/mediawiki/index.php?title=OpenSourceMalaria:Story_so_far&oldid=649790"