Most of the error in counting is due to floating of the regular coverslip when more sample is injected into the chamber (forceful rather than capillary action). If you decide to use regular coverslips, then do ensure that the coverslip is secured to the haemocytometer by applying water droplets on the bridges and slightly pressing the coverslip against the haemocytometer. This will ensure that the sample enters the chamber due to capillary action only!

What RNA extraction kit did you use? Did you blank the nanodrop with nuclease-free water?

Dear Olaf, I think you would like to get something like absolute value of something, but that does not exist. All things have only a relative value, and a numeraire is nothing else than an arithmetic unit, to simplify the calculation. In the majority of all economic models money plays no role, if you like all things can measured by a standard sheep. However, to make you maybe happy, then follow the following approach. It is no problem to calculate how long an average worker had to work to get a washing machine in 1950 and it is no problem to calculate the time which is needed by this average worker to get it today. If you do so, you will find out that the time has decreased dramatically and additionally the quality of a modern washing machine should also be taken into account, and that is real growth. However, the value of time measured in real goods has changed of course therefore. It is useless and senseless to search for an absolute value, others have done that a long time before you was born and we know all failed, because of missing consistency of arguments.

Admittedly this is not a new idea, but there are a few newer drugs that probably have not been investigated. I would look at drugs that target nuclei in the RAS. Many of those nuclei have diffuse projections to higher cortical areas and their output is highly regulated by autoreceptors. I would look at drugs that target those receptors and some of those drugs have already been suggested by others. One specific suggestion might be the locus coeruleus and alpha-2 adrenergic receptors. Methyldopa and clonidine were investigated for this very reason in the eighties, but with mixed success. However, a newer alpha-2 agonist dexmedetomidine which is more specific and potent might be better. I don't think anyone has used the approach you suggest with any one the newer agents currently available, so it is definitely a good idea.

Hi Martin, Thanks for pointing that out. So Do you mean to say the gate electrode and the drain electrode are somehow connected?But do you notice the point that the order of the current is very less(10^-8).

K20 should have EEC too - though you'll find things run faster with it disabled. Depends on how mission critical data integrity is (we've never had a noticeable problem through not having it enabled on our older Fermi cards, but we can run cheap checks on our answers so a random bit flip is not the end of the world for us). You should probably assess what code you want to run on the card before buying one. As you indicate not all cards are created equal. Be aware that this is especially true of Kepler cards that are almost two different architectures. There's the K10-equivalent cards that have poor double precision performance and lack many of the advanced features introduced on the newer K20-equivalent cores (things like warp shuffle and device-side kernel launches need the newer cores).

Oxygen is not necessarily replaced. The organism can undergo anaerobic respiration which produces an acid by-product which decreases affinity of hemoglobin to oxygen. However, in a decrease in oxygen levels, the affinity of hemoglobin to O2 can get lower as well. Please try to research for associationsbetween levels of partial pressure in blood oxygen and hemoglobin saturation. Also, if CO is present in the bloodstream, most likely, carbon monoxide poisoning can happen because it binds greater than oxygen.

Your question is about quantity, but I think you actually want to relate to appropriate ontologies. The Gellish project aims at supporting business and process models as well as product development and description. See also http://www.cmchr.net/Gellish-Ontology.html

Try Raman, you should see the softening of one (or more) of the lattice modes. Raman can give you decent signal even for micron size samples. Another way is to use Brillouin spectroscopy, but your sample has to be transparent and it is not so simple of a technique.

Hi, an explanation: The phenomenon can be understood by imagining two poisonous species that do not resemble one another and are also prey to a common predator. Occasionally, individuals of the predatory third species will encounter one or the other type of noxious prey, and thereafter avoid it. Predators that avoid only one or the other type of harmful species provide no benefit to individuals of the species that is not avoided. Therefore, there is an evolutionary advantage to be gained in the gradual approach in appearance of the two prey species. This is because a predator that learns to avoid either species in a pair of species exhibiting Müllerian mimicry learns, in effect, to avoid both. Cheers, Nadine

You could use ab against integrin or cadherin subunits. Just be carefull when selecting antibody because both have cytoplasmis domains

Its differ in crystal packing...of these solids....

Since the agency for which I work has a license to the software, I use various programs for developing maps or analysis products which includes ArcMap and ESRI. Concurrently I'm testing MatLab-image processing toolbox to leverage functions for raster images/spectral info management. Of greatest importance to me is the data collection prior to office data integration and management; there are specific qualities I'm trying to enhance in my workplace which relate to issues of scale at which certain phenomena are observed. Because of these scale-related issues I think its important to gain as precise and accurate information collected in the field as possible. These two qualities in data are enabled through Pathfinder Office (post-field GPS software) and TerraSync (GPS software). When properly configured, these software products enable the ability to record your PDOP (precision measure) as well as to develop data dictionaries (accuracy measure), which can be extremely useful if you have many different types of data to collect that include potentially long lists of information (ie. drop down menus for selection) or if you have a highly diverse user group in your workplace which fulfill various functions.

Hi Mary, To ask a question in this forum is easy- on top of the page you see the RG home, you will also see topic, publication, projects, more. Click on topic and you will find a page with spaces to write your question in short and elaborate versions.

this will occure one type of Banert cascade reaction....see this link... http://en.wikipedia.org/wiki/Banert_cascade https://www.thieme-connect.de/DOI/DOI?10.1055/s-2005-869892

http://en.wikipedia.org/wiki/Acid_dissociation_constant

As others have stated above, it depends not only on the drug and vehicle, but volume and frequency of administration. Is this going to be a single-dose, short-term acute or longer term treatment protocol? I'm mostly curious because Dex is a steroid, and lipophilic, and I'm wondering if it may partition to and remain longer in the fat pad than more hydrophilic compounds (especially following repeated doing). For example, when we inject 1g/kg ethyl carbamate in saline in 0.1mL i.p., we know that it has reached the bloodstream (and brain) within 1-2 minutes or so, because the anesthetic activity of that drug causes the animals to fall asleep. This is one example of a very small, very water-soluble compound. Your question pertains to not only a steroid, but a protein agent as well. As others have suggested, if the PK information regarding i.p. bioavailability of your compounds of interest are not generally available in the literature, the best way to know that your agents are in the blood is to measure plasma levels in a pilot study with a few animals. Then you will know how long it takes to get a X concentration in plasma, with X being the minimal concentration that you will accept for agent activity. You could also determine the time-to-peak and trough levels, and AUC, to find out what your therapeutic window will be. Many "inflammatory" stimulators work in phase, with immediate and delayed effects- will Dex affect both? Either? Will your planned experimental duration extend long enough to measure durable effects?

Cardiff University provide an e-Learning stand alone Masters level module on Research, Statistics and Evidence Based Practice, which is appropriate for different healthcare professionals working in any clinical areas. This might be something you're interested in developing further. http://courses.cardiff.ac.uk/postgraduate/course/detail/p280.html

There's a cheaper way. I don't if this was suggested already but you can use a jar with a candle inside which would deplete the levels of oxygen in the jar leaving carbon dioxide and some other minute gases. I hope this helps.

I like Halt from pierce it is a x100 solution, you can get the aliquoted in 100ul each single use 24x100ul. It has protease or protease and phosphatase inhibitors. With or without EDTA and The identity and concentration of each component is fully disclosed. http://www.piercenet.com/browse.cfm?fldID=02040806

Very interesting Steffen. Study available for perusal? Any speculation as to cause of disparity between follower/leader results?

You might consider also: Salvini, A., Faccio, E., Mininni, G., Romaioli, D., Cipolletta, S., & Castelnuovo G. (2012). Change in and through psychotherapy: a dialogical analysis single-case study of a patient with bulimia nervosa. Frontiers in Psychology, 3, 1-9. doi: 10.3389/fpsyg.2012.00546

thank you Francesca May be u r correct. I dont understand why this occure..here r my error out put GradGradGradGradGradGradGradGradGradGradGradGradGradGradGradGradGradGrad Berny optimization. Eigenvalue 91 is 6.84D-07 should be less than 0.000000 Eigenvector: D48 D46 D79 R2 A18 1 0.56625 -0.47827 0.23471 -0.18490 0.16703 A24 A2 D47 D90 A58 1 -0.15648 0.15630 0.14673 -0.12518 0.12093 Eigenvalue 92 is 5.66D-07 should be less than 0.000000 Eigenvector: D48 D79 R2 A18 A2 1 0.41866 0.31002 0.26634 -0.23572 -0.22591 D80 A58 A10 A59 A7 1 -0.20863 -0.19524 -0.17388 0.17099 -0.15644 Eigenvalue 93 is 4.93D-07 should be less than 0.000000 Eigenvector: D79 D46 D47 D80 D48 1 0.58073 0.40996 0.39478 -0.32123 -0.22400 A63 D98 R18 D96 D91 1 0.21079 -0.14580 0.09185 -0.08705 0.07816 Eigenvalue 94 is 2.08D-07 should be less than 0.000000 Eigenvector: D47 D46 D48 R19 R2 1 0.64127 -0.50320 -0.21995 -0.15577 0.14849 R18 A58 A2 A18 A64 1 0.13585 -0.13513 -0.12188 -0.11494 0.09223 NTrRot= -1 NTRed= 201 NAtoms= 32 NSkip= 111 IsLin=F Error in internal coordinate system. Error termination via Lnk1e in /usr/local/gaussian/g09/l103.exe at Mon May 20 20:45:29 2013. Job cpu time: 0 days 10 hours 42 minutes 9.4 seconds. File lengths (MBytes): RWF= 60 Int= 0 D2E= 0 Chk= 11 Scr= 1

This is a bit more formal and structured interaction then I would be comfortable with, but others can give their opinion.

Dear Junaid Ali, Mohamed El Jouad and Leke Olarinoye I have just send you the program Exoptic.exe, you must first install Visual Basic (VB40) or VB60 in order to determine the optical parameters from a transmission spectrum (in .dat format), I added a file (E2006.dat) on which you can practice before you master it. Best regards

Que bueno Miguel, si se te ofrece dime, yo tengo varias triple negativas aqui en EU. MDA-MB 468, Hs578t , MDA-MB 436, MDA-MB 453, MDA-MB 231. Tambien tengo varias, mas o menos otras siete que no son triple negativas. Suerte, Piedad