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Reaction Attempts Explorer

Two months ago I reported on the Reaction Attempts project and the availability of the summary as a physical or electronic (PDF) book. The basic idea behind the project is to collect organic chemistry reaction attempts reported in Open Notebooks. This would include not only successful experiments but also those which could be categorized as failed, ambiguous, in progress, etc.

The book was organized with reactants listed alphabetically. In this way one could browse through summaries of the types of reactions being attempted by different researchers on a reactant of interest. There might be information there (what to do or what to avoid) of some use for a planned reaction. At the very least one could contact the researcher to initiate a discussion about work that had not yet been published in the traditional system.

Andrew Lang has just created a web-based tool to explore the Reaction Attempts database in much more sophisticated ways.

Here are some scenarios of how one could use it. On the left hand side of the page is a dropdown menu containing an alphabetically sorted list of all the reactants and products in the database. Lets select furfurylamine.


This immediately informs us that there are 230 reactions involving furfurylamine and it lists the schemes for all these reactions upon scrolling down. That's still a bit hard to process so a second dropdown menu appears populated with a list of other reactants or products involved with furfurylamine.

We now select boc-glycine and that narrows our search to 145 reactions.

Selecting benzaldehyde from the third dropdown menu narrows the search further to 61 reactions.

The final dropdown menu contains a short list of only isocyanides and thus all represent attempted Ugi reactions. Selecting t-butyl isocyanide gives us 56 reactions.

That means that these same 4 components were reacted together 56 times. Looking at the various reaction summaries will show that some of these are duplicates for reproducibility and others vary concentration and solvent and the effect on yield is included. This particular reaction was in fact the subject of a paper on the optimization of a Ugi reaction using an automated liquid handler.

Now here is where the design of the Explorer comes in handy. We might want to ask if the reaction proceeds as well with the other isocyanides. All we have to do is switch the final dropdown menu to ask what happens when we go from t-butyl to n-butyl isonitrile. There is a single attempt of this reaction and it is "failed" in the sense that no precipitate was obtained from the reaction mixture. This doesn't mean that the reaction didn't take place - it might be that the Ugi product was too soluble. We can quickly inspect that the concentration and solvent are in line with conditions that allowed precipitation of the t-butyl derivative.

OK lets see what happens with n-pentyl isocyanide.

It looks like it behaves just like n-butyl isocyanide: another single non-precipitation event. What about benzyl isocyanide?

This time we do get the Ugi product from a single attempt. Note the lower yield compared to the t-butyl isocyanide under similar conditions.

What about with cyclohexyl isocyanide?

This time we hit an experiment in progress. A precipitate was obtained but it was not characterized. We can click on the link to the lab notebook page (EXP232) to learn more about how long it took for the precipitate to appear but there are not enough data to draw a definite conclusion about the successs of the reaction. However, based on the results from the other precipitates in this series it is probably encouraging enough to repeat and characterize the product.

There are other sources of information here. Clicking on the image of the Ugi product takes us to its ChemSpider entry. In this case the only associated data relates to this reaction attempt.

Lets look at another scenario: reactions involving aminoacetaldehyde dimethyl acetal.

In this case we find the intersection of two Open Notebooks. The first reaction comes from Michael Wolfle from the Todd group.

The second comes from Khalid Mirza from the Bradley group.

In order to learn more about the nature of the overlap we can use the substructure search capabilities of the Reaction Explorer. Simply click on the image of the acetal and the ChemSpider entry pops up. Now click on the copy button next to the SMILES for the compound.

Paste the SMILES into the SMARTS box of the Reaction Explorer.

We get 13 reaction attempts for this query - the two we found earlier and the rest corresponding to attempts by Michael Wolfle to synthesize praziquanamine.

We learn that one connection between these two notebooks involves different attempts at synthesizing praziquantel.

Hopefully this demonstrates the value of abstracting organic chemistry reaction attempts from Open Notebooks into a machine readable format. Contributions to the database require only the ChemSpider IDs of the reactants and product and a link to the relevant lab notebook page. Reaction schemes are automatically generated by the system. More on the Reaction Attempts project here.

Women’s Bioethics Project Closes

After six years of ground-breaking and influential blogging, the Women's Bioethics Project has come to an end. Kathryn Hinsch made the announcement on June 11.

For years, the WBP provided a crucial channel for female bioethicists to voice their concerns and support for key biotechnologies at the dawn of the transhuman era. Virtually no topic was off limits, whether it be voluntary euthanasia or the potential for exosomatic wombs. The WBP perspective was a breath of fresh air in a sea littered with bioconservatives, anti-technological feminists and religious conservatives. Not to mention overzealous male techno-optimists.

But it wasn't always this way. Back in 2003 I spoke at Yale about how feminists seemed to be forsaking the future, unwilling to engage in bioethical and biotechnological discourse. It seemed absurd to me at the time that the only people talking about such topics as human trait selection, reproductive technologies, genomics, and stem cell research were geeky white males (myself included). All feminists, it seemed to me at the time, were anti-technological ideologues who were unwilling to discuss the possibilities and what it might mean for women. Donna Haraway's legacy, I thought, had been all but abandoned.

It was with great relief, then, that the Women's Bioethics Project was launched a year later, featuring such writers as Linda MacDonald Glenn, Kristi Scott, Kelly Hills and many others. Indeed, as the blog header proclaimed, "This is not your typical blog. We have recruited scholars and public policy analysts from around the world to provide daily news and commentary on the implications of bioethical issues for women." And as Hinsch noted in her farewell post, "we developed innovative programs, policy recommendations and research on ethical issues pertaining to women’s health, reproductive technologies, and neuroethics. We made a difference: our work brought these important issues to new audiences and encouraged women to participate in policy development around bioethics questions."

And that they did. Their work will be missed, but thankfully many of the WBP alumni will continue to contribute to the IEET.

Well done, WBP!

Book: Choosing Tomorrow’s Children

Just added this to my ever growing must-read list: Choosing Tomorrow's Children: The Ethics of Selective Reproduction by Stephen Wilkinson. Here's an excerpt from Iain Brassington's excellent review:

In Choosing Tomorrow's Children, Stephen Wilkinson looks at the ethics of selection, concentrating mainly on 'same number' decisions that we may make. A 'same number' decision is one in which we have chosen to bring a child to birth, but have not decided which. (A 'different number' decision, by contrast, would be one in which we have to choose whether to reproduce at all.) Put another way, he is concerned with choosing between different possible future people (p5). Within this range, though, there's a number of different situations that may give us cause to want to choose: we might be making decisions about choosing an embryo to act as a 'saviour sibling', choosing an embryo to avoid a certain disability, choosing in favour of a (prima facie) disability - as in the case of Candace McCullough and Sharon Duchesneau, who sought specifically to have a deaf child - or choosing one gender over another. Wilkinson spends time considering all these variations on the 'choosing children' theme, and is guided by a presumption of permissibility - a presumption that everything is permitted unless and until it is forbidden, and that the onus is on the person doing the forbidding to make the case for impermissibility.

As far as Wilkinson is concerned, many (if not most) of the arguments that one might mount to establish the impermissibility of choosing children fail. This principle applies even in relation to controversial decisions such as McCullough and Duchesneau's. For in their case, the strongest argument that they would have to face would in all likelihood have to do with the welfare of the child created thereby: that deafness is welfare-reducing, and that it is wrong deliberately to created a child with lower welfare than it might otherwise have enjoyed. Yet, says Wilkinson, even this claim is weak. Partly this has to do with a scepticism about whether choosing for a disability is necessarily the same as choosing for a lower quality of life; partly it has to do with a claim that, even if disabled, people overwhelmingly have a life worth living, and that since this is the only life they could possibly have lived, there is no sense in which they could be said to suffer from a wrongful life; partly it is because the impersonal 'Same Number Quality Claim' - the idea that we ought to select for a higher quality of life whenever possible - does not reliably tell us that all examples of selecting for disability are wrong, and so, even at its strongest, will not tell us that this particular instance of choosing disability is de facto wrong.

Ethosuximide and valproic acid are more effective than lamotrigine in childhood absence epilepsy

Childhood absence epilepsy, the most common pediatric epilepsy syndrome, is usually treated with ethosuximide, valproic acid, or lamotrigine.

Ethosuximide and valproic acid are more effective than lamotrigine in the treatment of childhood absence epilepsy. Ethosuximide is associated with fewer adverse attentional effects.

References:
Ethosuximide, Valproic Acid, and Lamotrigine in Childhood Absence Epilepsy. NEJM, 2010.

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