International Journal of Pharmacy
International Journal of Pharmacy

... It is the post compression parameter which is used for the determination of Floating Lag Time/Buoyancy Lag Time (BLT) and Total Floating Time (TFT). The time required for the formulation to float on the surface of simulated gastric fluid from the time of introduction is called Floating Lag time / Bu ...
In vivo and in vitro metabolism studies of glaucine, a new
In vivo and in vitro metabolism studies of glaucine, a new

... of Glaucine in heterologically expressed single CYPs. The kinetic profiles were recorded for pHLM and all mainly involved CYPs by the metabolite formation approach. The results were compared with data of simple peak area ratios of analytes and internal standards. For testing the detectability, low d ...
2013_BJ_SCFBio_Website
2013_BJ_SCFBio_Website

... (1) "A Physico-Chemical model for analyzing DNA sequences", Dutta S, Singhal P, Agrawal P, Tomer R, Kritee, Khurana E and Jayaram B, J.Chem. Inf. Mod. , 46(1), 78-85, 2006; (2) “Molecular Dynamics Based Physicochemical Model for Gene Prediction in Prokaryotic Genomes “, P. Singhal, B. Jayaram, S. B. ...
Poster
Poster

... The Imig laboratory has helped develop EET analogs that mimic the actions of endogenous EETs, yet resist metabolism by sEH. The ability of the analogs to dilate the afferent arteriole in male rats was evaluated with renal vascular experiments. Blood pressure and heart rate were monitored using telem ...
SW_QA167_6Dosing_in_renal_impairmentFINAL
SW_QA167_6Dosing_in_renal_impairmentFINAL

... reported by different clinical laboratory creatinine measurement methods. Consequently, the results of pharmacokinetic studies on which this dosing information was based, were dependent upon the particular method for measuring serum creatinine used in a given study (9,26). However it is not possible ...
Guidance on CMC for Phase 1 and Phases 2/3 Investigational New
Guidance on CMC for Phase 1 and Phases 2/3 Investigational New

... ƒ Information on specific equipment, packaging and labeling process, in-process controls except for sterile products or atypical dosage forms not needed for Phase 2. Information on key equipment employed is needed for Phase 3 ƒ Reprocessing procedures and controls - safety related information for Ph ...
Drugs Shatter Lives
Drugs Shatter Lives

... • Death • There have been many cases where a drinker falls asleep, lapses into a coma and dies. Many times, the drinker is surrounded by friends, but help is not summoned because they are unaware of the severity of the drinker’s condition. Binge drinking, where drinkers consume excessive amounts of ...
Absorption
Absorption

... the drug is 100% bioavailable, 25% is metabolized and 75% is excreted as unchanged drug by the kidneys. If K=0.2/hr, Ka=1.5/hr, AUC=105.8 mg.hr/ml. Find Vd, total clearance, Cmax ,Xu∞. 7- Using the sigma-minus method of constructing urine data after the administration of 400 mg oral dose we found th ...
challenges in adc development
challenges in adc development

... Influence the ADC’s PK, therapeutic index and efficacy The ideal linker should be: • Stable so that the ADC does not release the cytotoxic drug before reaching its target, causing off-target toxicity. • Able to release the drug efficiently once internalized ...
Impact of Sample Preparation on Dissolution Testing: Drug Binding
Impact of Sample Preparation on Dissolution Testing: Drug Binding

... ignored, leading to inaccurate and irreproducible results. This paper discusses the effects of drug binding and extractable impurities from syringe filters on dissolution data. The data presented here demonstrate that various basic and acidic drugs bind strongly to nylon membrane filters, thereby re ...
A New Therapeutic Applications for Drug Repositioning
A New Therapeutic Applications for Drug Repositioning

... may be new uses for existing drugs as repositioning candidates have frequently been through several phases of development (ADMET, absorption, distribution, metabolism, excretion and toxicity; EMEA, European Medicines Agency; FDA, Food and Drug Administration; IP, intellectual property; MHLW, Ministr ...
Is There a Magic Bullet? - American Counseling Association
Is There a Magic Bullet? - American Counseling Association

... strength to which a drug binds to a receptor is known as affinity and the degree to which the drug activates that receptor is known as its intrinsic activity. Dissociation is the measure of disengagement from the receptor and is different from affinity. Dissociation, in part, accounts for the half l ...
Side Effects
Side Effects

...  Mechanism of action: by inhibiting 14 α demethylation affecting ergosterol synthesis in the cell membrane  Drug interactions are more with these groups because of the involvement of cytochrome P450 system ...
Ecstasy - Introduction to Health
Ecstasy - Introduction to Health

... associated with obtaining their next “fix” (the next dose and subsequent injection.) Those “associated activities” include burglary, robbery, prostitution, etc. to get money for their next fix. Physical Signs of Heroin Usage When someone has had a sufficient dosage, or from an hour to two hours afte ...
Snyder, Solomon H. - The Tanner Lectures on Human Values
Snyder, Solomon H. - The Tanner Lectures on Human Values

... for various medical purposes, almost all of which depended on its ability to block the actions of the neurotransmitter acetylcholine at various glands and muscles throughout the body. The interaction of acetylcholine with drugs provides an excellent example of both basic and applied science. Atropin ...
Carbamazepine VS Oxcarbazepine
Carbamazepine VS Oxcarbazepine

... • It is rapidly broken down to its pharmacologically active form which is then excreted through the kidneys. ...
adrenergic system - lec-4 2008
adrenergic system - lec-4 2008

... The plasma concentration of a B adrenoceptor blocking drugs have a complex relation ship with there effects , first order kinetic usually apply to elimination of the drug from the plasma. But there decline in the receptor block is zero order Most B adrenoceptor blocking drugs can be: 1- given orally ...


... Available in: http://www.redalyc.org/articulo.oa?id=243020634018 ...
Guidance for Industry
Guidance for Industry

... not create or confer any rights for or on any person and does not operate to bind FDA or the public. An alternative approach may be used if such approach satisfies the requirements of the applicable statutes and regulations. ...
enclosure-v
enclosure-v

... hypertension. Its oral bioavilibility approximately around 25-35%, because of its first pass metabolism and half life is about 6-8 h, respectively. Carvedilol is a off-white crystaline powder. Melting point is 114 to 1150C. Carvedilol practically insoluble in water (0.583 mg/L).3 Hence, there is a n ...
,
,

... analgesic is also known as painkiller, and is any member of the group of drugs used to achieve analgesia- relief from pain [1, 2, 3 and 4]. Analgesic drugs act in various ways on the peripheral and central nervous systems. They are distinct from anesthetics, which reversibly eliminate sensation, and ...
Topic D HL past paper questions 2011 (M10 – TZ2) Drugs can be
Topic D HL past paper questions 2011 (M10 – TZ2) Drugs can be

... (e) The structures of morphine and heroin are shown in Table 20 of the Data Booklet. Explain the increased potency of heroin compared to morphine. [2] 13. (M09- TZ1) Analgesics are used to relieve pain in the body. Aspirin and paracetamol (acetaminophen) are both mild analgesics. (a) Discuss the ad ...
Dissociation of a Diatomic Gas
Dissociation of a Diatomic Gas

... Let us consider the following simple model for a diatomic gas: a diatomic molecule consists of a pair of point-like atoms, each of mass m, separated by a rigid rod of length a. The rigid rod corresponds to the chemical bond, which requires an energy  to break. Now, at any finite temperature T , we ...
6. BRIEF RESUME OF THE INTENDED WORK: 6.1 NEED OF THE
6. BRIEF RESUME OF THE INTENDED WORK: 6.1 NEED OF THE

... and ``how much is there?'' continues to fuel the tremendous growth of LC-MS in the pharmaceutical industry. During this time, LC-MS has become widely accepted as an integral part of the drug development process. Integration of LC-MS in drug development: The significance is of two folds:  LC-MS has ...
SFINX—a drug-drug interaction database designed for
SFINX—a drug-drug interaction database designed for

... warnings of definite clinical relevance, avoiding any uncertainty with regard to administration routes, indication or dose range [16]. Practical advice on how to handle, monitor for, or circumvent a certain risk will hopefully also increase the compliance of prescribers. One of the major sources of ...

Drug design



Drug design, sometimes referred to as rational drug design or simply rational design, is the inventive process of finding new medications based on the knowledge of a biological target. The drug is most commonly an organic small molecule that activates or inhibits the function of a biomolecule such as a protein, which in turn results in a therapeutic benefit to the patient. In the most basic sense, drug design involves the design of molecules that are complementary in shape and charge to the biomolecular target with which they interact and therefore will bind to it. Drug design frequently but not necessarily relies on computer modeling techniques. This type of modeling is often referred to as computer-aided drug design. Finally, drug design that relies on the knowledge of the three-dimensional structure of the biomolecular target is known as structure-based drug design. In addition to small molecules, biopharmaceuticals and especially therapeutic antibodies are an increasingly important class of drugs and computational methods for improving the affinity, selectivity, and stability of these protein-based therapeutics have also been developed.The phrase ""drug design"" is to some extent a misnomer. A more accurate term is ligand design (i.e., design of a molecule that will bind tightly to its target). Although design techniques for prediction of binding affinity are reasonably successful, there are many other properties, such as bioavailability, metabolic half-life, side effects, etc., that first must be optimized before a ligand can become a safe and efficacious drug. These other characteristics are often difficult to predict with rational design techniques. Nevertheless, due to high attrition rates, especially during clinical phases of drug development, more attention is being focused early in the drug design process on selecting candidate drugs whose physicochemical properties are predicted to result in fewer complications during development and hence more likely to lead to an approved, marketed drug. Furthermore, in vitro experiments complemented with computation methods are increasingly used in early drug discovery to select compounds with more favorable ADME (absorption, distribution, metabolism, and excretion) and toxicological profiles.