Routes of Drug Administration
| | |
| |Oral |
| |Topical (Percutaneous) |
|Routes of Drug Administration |Rectal or Vaginal |
| |Pulmonal |
| |Parenteral |
| |Pills (single dose) |
| |Tablets |
| |Coated Tablets (shell) |
|Types of Orally Administered Drugs |Matrix Tablets (carrier meshwork) |
| |Capsules (gelatin shell) |
| |Troches/Lozenges |
| |Solutions |
| |Ointment + Lipophilic cream |
| |Paste |
| |Lotion |
|Percutaneous Drug Administration |Gels |
| |Can be single or multilayer, or contained in a reservoir |
| | |
| |Eye Drops |
| |Nose Drops |
|Other Topicals |Pulmonary Formulations |
| |Suppositories |
| |Ampules |
| |Vials |
| |Cartridge Ampules |
|Parenteral Drug Administration |Infusions |
| |Advantage: 100% Absorption, enters circulation without hepatic elim, better |
| |bioavailability of hydrophilic drugs |
| |External Absorption Barriers: (epithelial layer on skin, lung, intestine—Lipophilic |
| |barrier) |
|Types of Barriers for Drug Distribution/Absorption |Internal Blood-Tissue Barriers: Cardiac muscle, endocrine glands, gut, liver, CNS |
| |Passive Diffusion |
| |Active Transport |
|Drug Distribution |Receptor-mediated Endocytosis |
| |[DRUG] IS A FUNCTION OF ABSORBTION AND ELIMINATION! |
| | |
| |The AUC of the administered drug divided by the AUC of the intraveneously administered |
| |drug |
|Bioavailability |IV>TD>IM=SC>Rectal>Oral=Inhal |
| | |
| |Vd=Amt of drug in the mody/[drug] |
| |R of E: Via kidney (filtration) or liver (metabolism) |
|Volume of Distribution |Usually first order kinetics |
|Rate of Elimination |3 drugs have zero-order kinetics |
| |Rate of Elim/[Drug] |
| | |
| |Rate of Elim= k*Cp*Vd |
|Clearance |K= ln2/T ½ |
| | |
| |CL= K*Vd |
| |Convert parent compound into more polar metabolite |
|Phase I Reactions |Add/unmask functional group: |
| |OH, SH, NH2, COOH, etc |
| |Oxidation, Reduction, hydrolytic cleavage, Alkylation, Dealkylation, etc… |
| | |
| |Conjugation with endogenous substrate (increase aq solubility) |
| |Conjugation with gucoronide, sulfate, acetate, amino acid |
|Phase II Reactions | |
| |Require reducing agent and molecular oxygen |
| |Two enzymes: 1) Flavoprotein, NADPH-cytochrome c reductase |
| |2) Cytochrome P450 (electron acceptor); CYP |
|MFO | |
|Mixed Function Oxidases | |
| |PPAR ligands, CYP1, CYP2E, CYP2B |
| |Polymorphisms cause changes in drug metab: CYP2C19, CYP2B, CYP2D6 |
|P450 Enzymes |Induction of P450 enzymes=metabolize drug |
| |Glucoronidation |
| |Sulfation |
|Conjugation Reactions |Acetylation |
| |Amino acid Conj |
| |Glutathione Conj |
| |Fatty acid Conj |
| |Condensation Reaction |
| |Catalyze oxidative deamination of endogenous catecholamines (epinephrine) |
| |Lacated in never terminals and peripheral tissues |
| |Many drug/food interactions! (cheese, wine) |
|Monoamine Oxidases (MAO) |Inhib by MAO inhib |
| |Maximum non-toxic dose/Min effective dose |
| |Doesn’t take into account variability btw indivs |
|Therapeutic Index |LD50/ED50 |
| |Can be drugs or endogenous ligands for the receptor |
| |Increasing [agonist] will produce increase in biological response |
| |Full:evokes 100% max possible effect |
|Agonist |Partial: not 100% |
| |Block or reverse effect of agonist |
| |No effect on their own |
|Antagonist |Competitive, Non-competitive, inverse agonist (triggers neg response) |
| | |
| | |
| |Receptor |
|Four major drug targets |Enzyme |
| |Ion Channel |
| |Transporter |
| |Regulates many cellular and phys. Responses |
| |Gradient btw extracellular and intracellular (high:low) creates many opportunities for |
| |regulation |
|Ca++ as a Second Messenger |Stored in ER and other |
| |Voltage mediated: L, N, T |
| |Ligand gated |
| |Store operated |
|Ca Channels |Sesnsors: Annexins, EF-hand proteins, Calmodulin, ProponinC |
| |Target of many drugs! |
| |GPCR: transmembrane |
| |Bind GTP and GDP |
| |GAPS, GEFS, RGSs important in this regulation |
|G-Protein-coupled Receptors |Main Targets: Phospholipase C, Adenylate cyclase |
| |G-Proteins: Guanine nucleotide binding proteins |
| |2 groups: |
| |Small GTP binding |
|G-Proteins |Heterotrimeric G proteins |
| | |
| |Target of cAMP |
| |Four subunits (2 reg, 2 catalytic) |
|PKA |Phosphorylates transcription factors ex: CREB |
| |Heterologous desensitization (Incoming signal from different receptor) |
| |Homologous desensitization (only occurs on receptor which has already been stimulated) |
|Regulation of Receptors | |
| |Lipid soluble ligands that penetrate cell membrane, Receptors contain DNA-binding |
| |domains (transcriptional activators/suppressors) |
|Nuclear Receptors |Takes longer to act—requires penetration and protein synth first |
|GC, Mineralcorticoids, Retinoids PPARs | |
| |Common fatty acid chain+glycerol backbone+phosphor-residue |
| |PLA2 (reg through Ca++ and phos), PLC (Beta: Reg through GPCR, Gamma: EGFR or TCR, |
| |activated through tyrosine phosphorylation |
|Phospholipids | |
|Phospholipases | |
| |DAG: membrane bound, acts as a substrate for PLA2 |
|Phospholipases… |IP3: Ca++ regulated |
| | |
| | |
| |Eicosanoids: derivative of arachadonice acid |
| |Rapidly metab by COX into PG and LTs |
| |1st reaction: cyclic ring structure (COX), 2nd reaction: oxidation (Peroxidase) |
|Arachidonic Acid Metabolism | |
| |Vascular tone (relaxation, constriction) |
| |Platelet agg (Inc and Dec) |
|Function of PGs |Uterus tone (Inc) |
| |Bronchial Muscle (Contriction, relaxation) |
| |Gastric secretion (Inib), temp/pain |
| |LTC4, D4 and E4 mediate allergic rxn (SRS-A) |
| |Mediate anaphylactic shock, 10,000 more postent than histamine |
|Leukotrienes |Constricts bronchi, dilates bv |
| |LTB4 strong chemattractant for macrophage |
| |Divided into CNS and PNS |
| |PNS div into Somatic and Autonomous |
|Nervous System |Auto: Sypmathetic and Parasympathetic |
| |Muscarinic Receptors: Heterotrimeric G protein coupled, CNS, gastric mucosa M1 |
| |Cardiac=M2, Glandular=M3 |
|Cholinergic Receptors |Nicotinic Receptors: Ion channel coupled Muscle type, Ganglion type, CNS type |
| |Direct Parasympathomimetics: Affinity for M or N receptors (mimic Ach) |
| |Inderect Parasympathometics: Inhibit activity of Achesterase (Ach increased) |
| | |
|Cholinomimetics= | |
|Parasympathomimetics | |
| |Mimic Input |
| |Block Input |
|To affect Paraympathetic… | |
| | |
|To Treat associated diseases…. |Promote Parasymp |
| |Block Symp |
|Pilocarpine |Muscarinic Parasymp, does not activate N rec, treates glaucoma (local! Eyedrops) |
| | |
| |Muscarine has no therapeutic application! |
| | |
|Muscarine | |
| |Achestease Inhibitors, raise Ach |
|Carbamate |Physiostigmine (topical only) |
| |Neostigmine |
| | |
|Quaternary Alcohols |Edrophonium (diagnose Myasthenia Gravis) |
| |AcCh-ase inhib |
| |Acts as AcCh-ase inhib but active ingredient unkown |
| |Indirect stimulation of M3 receptor (vascular), triggers NO production=vasodilation |
|Horny Goat Weed |Action similar to Viagra (dangerous) |
| | |
| | |
|Ogranophosphates |AcCh-ase inhibitors (irreversible) |
| |No medical application |
|Nerve Gasses | |
| |Muscarinic Parasympathomimetic |
| |Atropine (antagonist of cholinergic system): CNS stimulant, before anesth. Prevent |
|Atropine |hypersecretion of bronchial mucus, treats bradycardy.. |
| |Hyoscine=CNS depressant, antiemetic, |
|Hyoscine | |
| |Competitive Antagonists: Compete with AcCh for N rec, prevent depolarization, |
| |reversible |
| |Agonists: Depolarizing blockers, AcCh mimetics not hydrolyzed by AcCh-ase, trigger a |
|Nicotinic Parasympatholytics |sustained depolarization, irreversible |
| |Dimeric AcCh, Acts as agonist like AcCh, not hydrolyzed by AcCh-ase (only plasma |
| |esterase) |
|Succinocholine/Suxamethonium |Depolarization triggers muscle twitching initially, |
| |Used for brief procedures |
| |AcCh: Preganglionic, parasyathetic post ganglionic neurons |
| |Norepinephrine: Most symp. Post ganglionic neurons (except sweat glands and renal |
|Transmitters in the Autonomic Nervous System |arteries) |
| |Epinephrine (adrenalin): Adrenal medulla--symp impulses (no gang) |
| | |
| |Reuptake into presynaptic nerve ending |
|Termination of (Nor)epinephrine action |Catechol-O-methyltransferase |
| |MAO |
| |Presynaptic alpha 2 receptors |
| |Alpha1 (vasc smooth muscle) |
| |Alpha 2 (presynaptic) |
|Adrenergic Receptors |Beta 1 (Heart) |
| |Beta 2 (repiratory, uterine SM cells) |
| |Beta 3 (Adipocytes) |
| |MAO-Inhibitors |
| |Indirect Sympathicomimetics |
| |Inhib of MAO causes increase in free Nor-Ep, in CNS NAO metab dopamine and serotonin |
|Tranylcypromine |(inhib=increase in happy hormones) |
|Moclobemide | |
| | |
| |Indirect Sympathicomimetics |
| |Displace nor-E in storage vesicles=forced release of NorE |
|Ephedrine |Dietary Supplements |
| |Indirect Sympathomimetics |
|Amphetamines |Displace norE in storage vesicles, forced release, inhib NorE re-uptake and deg by MAO |
|Methylphenidate |(TRIPPLE ACTION), Meth=ADD, Fen=Appetite suppressant, Meta=more lipophilic, depletes |
|Fenfluramine |NorE |
|Metamphetamine | |
| | |
| |Non-selective Agonists |
|Epinephrine |Sympathomimetics |
| |Ep: Activates alpha and beta rec |
|Norepinephrine |Blood pressure increase, dilates bronchii, vasopressor, Treat anaphylactic shock |
| |NorE: alph receptors, increase BP, potent vasopressor |
| |Alpha1 selective agonist |
|Methoxamine |Sympathomimetics |
|Phenylephrine |Methoxamine: treatment of hypotensive state |
|Naphazoline |Phen: Local vasoconstrictor, nasal decongestant |
|Oxymetazoline |Zoline=alpha 1 |
|Xylometazoline | |
| |Alpha 2 selective agonist |
| |Produce sympatholytic effect, but sympathomimetics! Actviate presynaptic a-2 rec in |
| |cardiovascular control in the CNS |
|Clonidine |BP decrease |
|Guanfacine | |
| | |
| |B1-selective agonist, stimulate heart |
| |Strgon inotropic effect, little chronotropic effect, short term treatment of impaired |
|Dobutamine |cardiac function |
| |B2 selective agonist |
|Metaproterenol |Treat asthma, non-selective sympathomimetics |
|Albuterol |Differ in speed and onset, duration of action |
|Formoterol | |
| |Indicated for pheocromocytoma. |
| |Blocking α1 causes vasodilation; reducing BP |
|Non-selective Blockers |Blocking α2 removes inhibition, increasing NE action on β receptors ( increasing HR and |
|Phentolamine |cardiac output |
| | |
| |Selective α1 Blocker |
|Prazosin, Terazosin, etc |Indicated for hypertension and urinary retention. |
| |Side effects: Reflex tachycardia and postural hypotension |
| | |
| |Selective α2 Blocker (sympathomimetic!) |
|Yohimibine |Increases sympathetic outpout. Used for male sexual dysfunction and as a weight loss |
| |drug |
| |Noncardioselective β blockers |
| |1st gen. drug, cross reaction w/ β2 causes bronchoconstriction |
|Propranolol |Labetalol also blocks α1 receptors (strong antihypertensive drug) |
| |same indications as cardioselective blockers |
| |Cardioselective β blockers |
| |Newer drugs are more β1 selective. |
|Metoprolol, Atenolol… |Indicated for angina pectoris, hypertension, cardiac dysrhythmias, myocardial |
| |infarction, heart failure, and stage fright (anxiolytic). |
| | |
| |CNS/ANS (decrease symp. tone) |
|Potential targets of Antihypertensive drugs |Heart: decrease cardiac output |
| |Veins: Dilate, decrease preload |
| |Arterioles: dilate, decrease afterload |
| |Kidneys: increase diuresis |
| |Calcium channel blockers (antagonist) |
|Dihydropyridines: |Inhibit Ca entry into cells of arteries |
|Nifedipine, Nicardipine, Nimodipine… |Targets specifically L-type channels on VSMC, no cardiac effect |
| |Can cause peripheral edema |
|Minoxidil |Potassium Channel Agonists |
| |Increases membrane permeability to K+, K+ efflux causes membrane hyperpolarization, |
| |inhibiting voltage gated Ca2+ channels ( relaxation of smooth muscles ( vasodilation ( |
| |reduces BP |
| |Side effect: hair growth (Rogaine) |
|Nitroprusside |Vasodilator |
| |Delivered thru iv only and is metabolized into NO which directly activates cGMP |
| |production ( vasodilation, Rapid action! |
| |(Caffeine & Viagra) |
| |Hypertensive Emergencies! |
| |ACE-Inhibitors, angiotensin I not converted into the active peptide (ATII), no |
|Captopril |aldosterone & ADH release ( no fluid retention |
|Enalapril |-no sympathomimetic effects |
|Benazepril |-no vasoconstriction |
|Lisinopril |Side effect – causes coughing |
| |Angiotensin II (ATII) Receptor Blocker |
| |Inhibits the effect of AT II by blocking the receptor |
|Losartan |usually used if patient cannot tolerate the cough caused by ACE inhibitors |
|Candesartan | |
|etc… | |
|Stable Angina |Predictable episodes; usually during/after physical exertion or stress. Treatment: |
| |Nitrates & β-Blockers (Propranolol, etc.) |
| | |
|Unstable Angina |Chest pain unexpected and usually occurs at rest |
| |Treatment: Nitrates |
| | |
|Variant Angina |Chest pain almost always occurs at rest. Due to coronary artery spasm. Treatment: |
| |Calcium channel blockers (Nifedipine, etc…) |
| |Treats angina pectoris. Reduces cardiac workload (and its oxygen demand) by reducing |
| |venous return. Causes vasodilation primarily in veins. Oral, sublingual, IV, Buccal |
| |and Transdermal ROA |
|Nitroglycerine |Do not combine w/ other vasodilators (Viagra) |
|Isosorbide-dinitrate |More stable than nitroglycerine |
|(ISDN) |Tolerance can occur, give lowest dose |
| |Do NOT combine w/ other vasodilators |
| | |
| |Promotes peripheral vasodilation. |
|Nitroprusside |IV only; rapid onset and short duration – allows for titration |
| |Sodium Channel Blockers |
| |Slows depolarization phase of AP. |
|Arrythmia Treatment |Procainamide – used for atrial & ventricular arrhythmias |
|Class I |Lidocaine – used for acute ventricular arrhythmias |
| |Flecainide – used for chronic treatment of ventricular arrhythmias |
| | |
| | |
|Arrythmia Treatment |β-Blockers |
|Class II |Propranolol |
| |used for tachycardia |
| | |
| | |
|Arrythmia Treatment |Potassium Channel Blockers |
|Class III: |Prolongs repolarization by blocking potassium efflux. |
| |Bretylium & Amiodarone |
| |used for intractable ventricular arrhythmias |
|Class IV: |Prolongs repolarization by blocking calcium influx |
|Calcium Channel Blockers |Verapamil – blocks both L & T Type calcium channels! |
| |Blocking T Type channels ( slows conduction |
| |(Blocking L Type channels ( coronary + arterial vasodilation) |
| | |
| | |
| |Adenosine – for paroxysmal supraventricular tachycardia |
| |Digoxin – atrial fibrillation |
|Other Cardiac Arrythmia Drugs |Epinephrine - bradycardia |
| |Inadequate contractility; ventricles unable to expel blood ( rise in venous blood |
| |pressure. Caused by blocked coronary arteries, viral infections, hypertension, leaky |
| |heart vavles, myocardial infarction |
|Congestive Heart Failure |Right sided failure – lower limb edema, Left sided failure – pulmonary edema & |
| |respiratory distress |
|Cardiac Glycosides |Slows heart rate and increases contractility. |
|(Digoxin) |Inhibits Na/K ATPase, leading to an increase intracellular Na+, Increased Na+ slows |
| |Na/Ca exchanger, leading to an increase intracellular Ca++. Low therapeutic index. |
| |Potassium competes with digoxin in binding to Na/K ATPase |
| | |
| |Reduces cardiac workload, inhibits vasoconstriction, inhibits sodium/fluid retention, |
|ACE inhibitors & |inhibits NE release |
|ATII antagonists | |
| | |
|Captopril & Losartan | |
| | |
| | |
|Vasodilators |Nitrates: Nitroglycerine, etc. (review Nitrates notes) |
| | |
| | |
|Carbonic Anhydrase Inhibitors |Inhibits conversion of CO2 ( (H+) + (HCO3-), blocking reabsorption of Na+ |
|Azetazolamide |-Usually indicated for Glaucoma |
|Dorzolamide |Causes metabolic acidosis (lower HCO3-) |
| |Inhibits Na+/K+/2Cl- symporter at ascending limb in the Loop of Henle; blocking Na, K, |
| |Cl reabsorption |
|Loop Diuretics (high ceiling) |most potent diuretic |
|Furosemide |for severe/moderate hypertension & edema |
|Torasemide |Causes hypokalemia |
| |Inhibits Na+/Cl- symporter at distal convoluted tube |
| |Used for moderate hypertension & heart failure (edema) |
|Thiazide Diuretics |Causes hypokalemia |
|Hydrochlorothiazide | |
|Benzthiazide | |
| |Acts as distal portion of distal tube; enhances Na excretion & reduces K excretion |
| |Spironolactone – aldosterone receptor antagonist (slow) |
|Potassium-Sparring Diuretics |Amiloride – directly blocks Na/K channel (fast) |
|Spironolactone |Used in combo w/ other diurectics |
|Amiloride | |
| |Non-reabsorbable molecules that inhibit passive reabsorption of water (promoting water |
| |excretion w/ little Na excretion), does not cross blood-brain barrier, so water goes |
|Osmotic Diuretics |from brain to blood, Used to reduce intracranial pressure, IV only |
|Mannitol | |
| |Indicated for kidney stones and gouts. |
| |Therapeutic dose: promotes excretion and inhibits reabsorption of uric acid |
|Uricosuric Agents |Sub-therapeutic dose: inhibits both excretion and reabsorption |
|Probenecid |Strongly inhibits penicillin excretion which is good if need long lasting penicillin |
| |performance |
| |Neutralizes stomach acid. |
|Weak Bases: |Magnesium Hydroxide – causes diarrhea |
|Aluminum Hydroxide |Aluminum hydroxide – causes constipation |
|Magnesium Hydroxide |Often combined to reduce side effects of each |
|PeptoBismol, Tums | |
| |Competitively inhibits binding of histamine to H2 receptors on parietal cells; reduces |
| |histamine stimulated gastric acid production |
|H2 Receptor Blockers: | |
|Cimetidine | |
|Ranitidine | |
| |Irreversible inhibition of H+/K+ ATPase in parietal cells |
|Proton Pump Inhibitors: |Only active at low pH (activity restricted to stomach) |
|Omeprazole |Inhibits acid production for 1-2days |
|Lansoprazole |Does not neutralize acid in stomach, only prevents production |
|Esomeprazole | |
|Rabeprazole | |
| | |
|Mucosal Protective Agents: |Misoprostol: PGE analog; stimulates mucus and HCO3 production |
|Misoprostol |Combined w/ NSAIDS |
|Sucralfate |Sucralfate: stabilizes mucus to inhibit H+ diffusion, not absorbed |
| | |
| |H1 Antagonists |
| |Muscarinic receptor antagonists |
|Antiemetic Drugs: |Benzodiazepines |
|Potential Treatment Options |D2 antagonists |
| |Cannabinoids |
| | |
|H1 Antagonists |Diphenhydramine, Meclizine, etc |
| |Blocks H1 (histamine) receptors competitively |
| | |
| |Scopolamine (anticholernergic) |
|Muscarinic Receptor Antagonists | |
| |Lorazempam; potentiates effects of GABA in CNS |
|Benzodiazepines | |
| | |
| | |
|D2 (dopamine) Antagonists: |Competitively blocks C2 receptors in the CTZ |
|Metoclopramide |Increases gastric emptying |
|Domperidone |Contraindicated in patients w/ Parkinson’s disease |
| | |
| | |
| |Synthetic cannabinoids: Nabilone, Dronabinol |
|Cannabinoids | |
| |Acts as agonist at cannabinoid receptors in the CNS |
|Bulk Laxatives |Increases bowel content volume triggering stretch receptors |
| | |
| |Insoluble, expands with water |
|Carbohydrate Based |May cause constipation if not enough water |
|Vegetable Fibers, Bran | |
| |partially soluble/non-absrobable |
|Osmotically Active |potent and fast acting |
|Epsom salt | |
|Glauber’s salt | |
|Irritants: | |
|Ricinoleic acid (Castor Oil) |Castor oil converted to ricinoleic acid |
| |works in the small intestine |
| | |
|Anthraquinones | |
|Diphenolmethanes |Works in the large intestine |
|Bisacodyl | |
|Sodium picosulfate | |
| | |
| |Longer interval needed to refill colon, most common cause of constipation |
| |Loss of water/salt in gut leads to aldosterone release |
| |Causes excretion of K+ |
|Laxative Abuse | |
| |Opiod derivative that selectively acts in the GI tract (w/no CNS activity) |
| |Acts on the intestinal muscles reducing motility=increase in water and electrolyte |
|Antidiarrheal: |reabsorption |
|Loperamide |Dimethicone: anti-gas agent that is often combined with anti-diarrheal drugs |
|(Imodium) | |
|Insulin (unmodified) |short acting |
| |only insulin that can be administered thru iv |
| | |
| |rapid onset and short acting |
|Insulin Lispro (Humalog) | |
| |SC injection only, insulin + zinc ( micro-precipitates delayed absorption |
| |long lasting, UltraLente = longest lasting |
|Insulin Lente | |
| |SC injection only, insulin + zinc ( micro-precipitates delayed absorption |
|Insulin Lente |long lasting, UltraLente = longest lasting |
| | |
| | |
| |insulin + protamine (delayed absorption |
|NPH Insulin |long lasting |
| | |
| |Synthetic insulin that is soluble at low pH, but becomes insoluble and forms |
| |precipitates at neutral pH after SC administration |
|Insulin Glargine |long lasting (similar to Lente) |
|Lantus | |
| | |
|Sulfonylureas |Stimulates insulin release; useful for diabetes caused by low insulin levels where β- |
|Tolbutamide (1st gen.) |pancreatic cells are still present |
|Glimepiridide | |
|Glipizide | |
| | |
|Glitazones |Increases insulin sensitivity at target cells |
|Rosiglitazone |Acts as a nuclear hormone receptor (PPARγ agonist) increasing transcription of insulin |
|Pioglitazone |receptor signaling components and glucose transporters |
| | |
| |Unknown mechanism |
| |Increases glucose uptake & inhibits gluconeogenesis |
|Biguanides |Lowers LDL and VLDL |
|Metformin |Suppresses appetite |
| |No hypoglycemic effects |
| |Reversible HMG-CoA Reductase inhibitors. HMG-CoA reductase is the rate-limiting enzyme |
| |in the production of cholesterol. Inhibition effectively reduces de novo synthesis of |
|Statins |cholesterol precursors. |
|Lovastatin |Lower cholesterol levels upregulates LDL receptors in liver removing LDL from the |
|Atorvastatin (Lipitor) |bloodstream |
| |PPARα agonists – stimulates β-oxidation of fatty acids |
| |Promotes lipoprotein lipase activity |
|Fibrates |Lowers VLDL (minor effect on LDL) |
|Clofibrate |Increases HDL levels |
|Benzafibrate | |
| |Bile acid binding resins prevent reabsorption of bile acids in enterohepatic |
| |circulation, Increases cholesterol synthesis to make more bile acid-plasma cholesterol |
|Resins |levels remain unchanged. The liver also upregulates LDL receptors to increase hepatic |
|Cholestyramine |uptake of LDL (reducing plasma LDL) |
|Colestipol | |
| | |
| |Inhibit all phases of inflammation, inhibits NFκB, upregulates lipocortin (lipocortin |
| |inhibits PLA2, =no PT or LT synthesis, promotes fetal lung development by increasing |
|Glucorticoids (GCs) |surfactant |
|Addison’s Disease |Adrenal cortex failure, Lack of GC production |
| | |
| |Adrenal cortex tumors, GC overproduction |
|Cushing Syndrome | |
| | |
| |=Cortisol, main GC in humans |
| |Used for adrenal insufficiency (Addison’s Disease) |
|Hydrocortison |mostly topical application |
| |Binds with mineralcorticoid receptors |
| |Have Na retaining effects |
|Prednisone |Pro-drug; converted to active form (prednisolone) |
| | |
|Prednisolone |Drug of choice for systemic administration |
| |Lower Na retaining effects |
| |Stronger anti-inflammatory than cortisol |
|Triamcinoline |No Na retaining effect |
| | |
| |Betamethasone, Dexamethasone: 30x more potent than cortisol, no water or Na retaining |
|Halogenated GC |effects |
|Estrogens: |Produced from andgrogen precursors |
| |Estradiol=primary estrogen in human, breast devel, bone density, growth of uterus, |
|Estradiol |increase HDL, etc., no oral admin (1st pass hepatic elim) |
| | |
|Estrone |Estriol only during pregnancy |
| | |
|Estriol | |
|Ethinylestradiol |Most widely used |
| |Induce expression of progesterone receptors, Progesterone inhib expression of estrogen |
| |receptors |
| | |
| |Oral contraceptive |
|Diethyl-Stilbestrol | |
|Raloxifene |Indicated for postmenopausal osteoporosis, Selective estrogen receptor modifier (SERM), |
| |Anti-estrogenic effect on breast and endometrium, Estrogenic effect on bone and lipid |
| |metabolism |
| | |
| |Oral contraceptives, prodrug |
| | |
|Mestranol | |
| | |
|Tamoxifene | |
|(antiestrogen) |Indicated for breast cancer |
| |anti-estrogenic effect on breast tissue |
| |weak effect on bone and lipid metabolism |
|Progesterones: |Inhibits rhythmic contractions of myometrium, not for oral admin (1st pass elim) |
| | |
|Progesterone | |
| |Stable derivatives |
|Hydroxyprogesterone | |
| | |
|Medroxyprogesterone | |
| | |
|Progesterone | |
| |Testosterone derivatives with progesterone activity |
|Norethindrone | |
|Norgestrel | |
|Desogestrel | |
| |1980s French company, found that it blocks progesterone receptors, induces abortion |
|Anti-Progesterones |Addition of small doses of prostaglandin analogue few days later stimulates uterine |
|Mifepristone |contractions=very efficacious for termination of pregnancy |
|Testosterone |Responsible for both anabolic and androgenic effects |
| |Rapidly metabolized by the liver. |
| |-ester derivatives increases its half-life |
| | |
|Nandrolone |Strong anabolic effects, Injection only |
|(banned) | |
| | |
| | |
|Stanozolol |Strong anabolic effects (Not a β blocker!) |
|(banned) |Oral admin |
| |Dehydroepiandrosterone. Marketed as an anabolic steroid |
| |Misleading b/c it’s a precursor for both testosterone and estrogen. |
|DHEA |High levels of DHEA may lead to elevated levels of testosterone and estrogen. |
| | |
| | |
|Flutamide |Used to treat prostate cancer |
| |Competitive androgen receptor antagonist |
| |Blocks testosterone stimulating effects |
| | |
| |Treats prostate gland enlargement and baldness, blocks the conversion of testosterone to|
|Finasteride |DHT (testosterone metabolite that is much more potent) |
| |Bald men have elevated levels of DHT |
| | |
| |Treats endometriosis (growth of endometrium outside of the uterus) |
|Danazol |Inhibits GnRH release, no LH/FSH production=no steroid production |
|Synthetic GnRH |Given in pulses (s.c.), induced ovulation (stimulates LH/FSH) |
|-Gonadorelin |Given continuously, medical castration (desensitize GnRH receptors) |
|-Buserelin | |
| |Bile acid binding resins prevent reabsorption of bile acids in enterohepatic |
| |circulation, Increases cholesterol synthesis to make more bile acid-plasma cholesterol |
|Resins |levels remain unchanged. The liver also upregulates LDL receptors to increase hepatic |
|Cholestyramine |uptake of LDL (reducing plasma LDL) |
|Colestipol | |
| | |
| |Inhibit all phases of inflammation, inhibits NFκB, upregulates lipocortin (lipocortin |
| |inhibits PLA2, =no PT or LT synthesis, promotes fetal lung development by increasing |
|Glucorticoids (GCs) |surfactant |
|Addison’s Disease |Adrenal cortex failure, Lack of GC production |
| | |
| |Adrenal cortex tumors, GC overproduction |
|Cushing Syndrome | |
| | |
| |=Cortisol, main GC in humans |
| |Used for adrenal insufficiency (Addison’s Disease) |
|Hydrocortison |mostly topical application |
| |Binds with mineralcorticoid receptors |
| |Have Na retaining effects |
|Prednisone |Pro-drug; converted to active form (prednisolone) |
| | |
|Prednisolone |Drug of choice for systemic administration |
| |Lower Na retaining effects |
| |Stronger anti-inflammatory than cortisol |
|Triamcinoline |No Na retaining effect |
| | |
| |Betamethasone, Dexamethasone: 30x more potent than cortisol, no water or Na retaining |
|Halogenated GC |effects |
|Estrogens: |Produced from andgrogen precursors |
| |Estradiol=primary estrogen in human, breast devel, bone density, growth of uterus, |
|Estradiol |increase HDL, etc., no oral admin (1st pass hepatic elim) |
| | |
|Estrone |Estriol only during pregnancy |
| | |
|Estriol | |
|Ethinylestradiol |Most widely used |
| |Induce expression of progesterone receptors, Progesterone inhib expression of estrogen |
| |receptors |
| | |
| |Oral contraceptive |
|Diethyl-Stilbestrol | |
|Raloxifene |Indicated for postmenopausal osteoporosis, Selective estrogen receptor modifier (SERM), |
| |Anti-estrogenic effect on breast and endometrium, Estrogenic effect on bone and lipid |
| |metabolism |
| | |
| |Oral contraceptives, prodrug |
| | |
|Mestranol | |
| | |
|Tamoxifene | |
|(antiestrogen) |Indicated for breast cancer |
| |anti-estrogenic effect on breast tissue |
| |weak effect on bone and lipid metabolism |
|Progesterones: |Inhibits rhythmic contractions of myometrium, not for oral admin (1st pass elim) |
| | |
|Progesterone | |
| |Stable derivatives |
|Hydroxyprogesterone | |
| | |
|Medroxyprogesterone | |
| | |
|Progesterone | |
| |Testosterone derivatives with progesterone activity |
|Norethindrone | |
|Norgestrel | |
|Desogestrel | |
| |1980s French company, found that it blocks progesterone receptors, induces abortion |
|Anti-Progesterones |Addition of small doses of prostaglandin analogue few days later stimulates uterine |
|Mifepristone |contractions=very efficacious for termination of pregnancy |
|Testosterone |Responsible for both anabolic and androgenic effects |
| |Rapidly metabolized by the liver. |
| |-ester derivatives increases its half-life |
| | |
|Nandrolone |Strong anabolic effects, Injection only |
|(banned) | |
| | |
| | |
|Stanozolol |Strong anabolic effects (Not a β blocker!) |
|(banned) |Oral admin |
|Combination Pills |Highly effective, Estrogen component: Ethinylestradiol, Progesterone component varies |
| |Biphasic preparation – includes progesterone break after 7 day break |
| |Monophasic preparation – no progesterone break (but [progesterone] varies throughout |
| |cycle) |
|Mini Pill |Less reliable than combination pills |
| |Contains only progesterone, used when estrogen is contraindicated |
| |Contraception mechanism relies mainly on increased mucus viscosity. |
| |-mucolytic agents (cough medications) may cause contraception failure |
| | |
| | |
|Morning After Pill |High dose of progesterone |
|Levonorgestrel |Must be taken within 72 hours of sexual intercourse |
|Dephenhydramine |H1 antagonists (antihistamine), 1st generation |
|(Benadryl) |Indicated for seasonal and skin allergies |
| | |
| |Anti-emetic |
|Dimenhydrinate |Also blocks mAChRs |
|(Dramamine) | |
|Doxyamine |H1 antagonist, 1st generation |
|(Nyquil) |Most potent OTC sedative (better than barbiturates) |
| |Same efficacy as diphenhydramine in terms of anti-allergies |
| | |
| | |
|Clemastine | |
| |1st generation H1 antagonist |
|Chlorpheniramine |Also anti-depressant (inhib serotonin uptake) |
| | |
| |Antiemetic (less drowsiness) |
|Meclizine | |
| |Antihistamine due to metabolite |
|Hydroxyzine | |
|Cetrizine |2nd generation H1 antagonist |
| | |
|Loratadine |No entry to CNS, no drowsiness T ½=8 hr |
| | |
|Desloratadine |Longer T ½ |
| | |
|Fexofenadine |Highly selective for H1 receptor |
|Cromolyn | |
| |Mast cell stabilizer |
| |Prevents asthma, does not stop attack |
|Nedocromil |Prevents mediator release from mast cells |
| |Inhalation or eye drops |
|Montelukast (Singulair) |Leukotriene Receptor Blockers |
| | |
| |Prevents exercise and aspirin-induced asthma |
| |Antagonist of LTD4 at cysteinyl LT receptor |
| | |
|Zileuton (Zyflo) |5-Lipoxygenase Inhibitor |
| | |
| |Prevents production of all leukotrienes |
| |Not useful for treatment of attacks |
|Barbiturates |General inhibition of the CNS w/ |
| |sedative-hypnotic actions Augments |
| |GABA responses (by potentiating GABA |
| |signal) and mimics GABA (by opening |
| |Cl-channels in the absence of GABA). |
| |Keeps Cl channels open longer, |
| |hyperpolarizing the cell preventing |
| |further excitation. Alsoblocks excitatory |
| |glutamate receptors |
|phenobarbital |Barbituates |
| |epilepsy (phenobarbital) and anesthesia induction (thiopental) |
|thiopental |Side effects/Risks: |
| |high risk of dependence (severe/lethal withdrawal symptoms) |
|Amobarbital |may lead to cardio-respiratory depression |
|Pentobarbital |potent inducers of P450 enzymes; drug interactions (contraceptives, etc.) |
|Secobarbital | |
|Benzodiazepines |Seven-membered ring fused to aromatic ring, Selective activates GABA receptor operated |
| |Cl channels, Increase affinity of GABA for rec., Treat Anxieties, fewer side effects |
|Chlordiazepoxide, Diazepam, Lorazepam, Flunitrazepam, Alprazolam, Triazolam |than barb., anterograde amnesia |
|MAO Inhibitors as Antidepressants |Increase norepinephrine, serotonin, and dopamine (prevents metab) |
|Tranylcypromine |Side effects high |
|Phenelzine |Food-drug interaction: cheese |
|SSRIs |Increase serotonin levels by preventing neuronal reuptake |
| |Same efficacies as TCAs, fewer side effects |
|Fluoxetine |Inhib sexual climax, can cause aggression |
|Paroxetine | |
|Sertraline | |
|Clotalopram | |
|Tricyclic Antidepressants |Increase norepinephrine and serotonin by preventing neuronal reuptake, strong |
|Imipramine |interaction with alcohol. Sedation=side effect |
|Desipramine | |
|Clomipramine… | |
|Phenothiazines |Treat Schizophrenia |
| |1st gen: neuroleptic |
|Butyrophenones |Block dopamine receptor on post synaptic vesicle, Cause acute dystoni, akathesia, |
| |tardive dyskinesia, sedation, dry mouth, lactation, interaction with alcohol |
|Clozapine |Atypical Neuroleptics (2nd gen) |
| |Inhibit 5-HT and D2 receptors, act mostly on limbic system, not in striatum (fewer side |
|Olanzapine |effects) |
|L-dopa (Levodopa) |Treat Parkinsons Disease |
| |Metabolic precursor of dopamine, often combined with Carbidopa (LDOPA decarboxylase |
|Carbidopa |inhib). Increases amt of L-Dopa that reaches the brain |
|Bromcriptine |Dopamine Agonists |
| |Similar to L-dopa |
|Pergolide |D2 agonists, treat Parkinsons |
| | |
|Pramipexole | |
| | |
| |Inhib of MAOb, extends half-life of dopamine, Indirect dopamine agonists, Treats |
| |Parkinsons, also antidepressant |
|Selegiline | |
| |Muscarinic acetylcholine receptor antagonist. |
| |Reduces cholinergic signals in the CNS (responsible for stimulating GABA output |
|Atropine |suppressing the thalamus) |
| | |
| |No longer used for Parkinson’s disease |
| |Blocks voltage gated Na channels that are in the inactivated state, preferentially |
| |blocks high frequency discharges. (use-dependent inhibition) |
| |(does not elevate seizure threshold, limits the propagation and spread of seizure), Zero|
|Phenytoin |order kinetics, Indicated for convulsive seizures, Side Effect: hyperplasia |
| |Treats Epilepsy, inhib of ca channels, |
|Ethosuximide |Etho=blocks T-type channels, drug of choice for absence seizures |
| | |
|Valproate |Val=mech unclear, good for convulsive and absence seizures |
| |Hepatotoxic |
| |Treats alcholoism |
| |inhibits aldehyde dehydrogenase; leading to acetylaldehyde accumulation causing |
| |“hang-over” |
|Disulfuram |-also blocks the conversion of dopamine to NE, rise in dopamine levels causes |
| |schizophrenic symptoms |
| | |
| | |
|Naltrexone |Treats Alcoholism |
| |opiod receptor antagonist; inhibiting the reward response that normally results for |
| |alcohol consumption |
| |IV anesthetic |
| |Rapid onset with high lipid solubility (accumulates in fat); slow recovery |
|Thiopental |Narrow therapeutic range |
|(barbiturate) |No analgesic effect |
| |IV anesthetic |
| |Rapidly metabolized for quick recovery. |
|Propofol |Used for same-day surgery |
| |IV anesthetic |
| |Phencyclidine (PCP) analogue; may cause hallucinations during recovery |
|Ketamine |Have both anesthetic and analgesic properties |
| |-often used in veterinarian medicine and in tranqulizers |
| |IV anesthetic |
| |Benzodiazepine. Very short-acting. |
|Midazolam |Have all benzodiazepine properties, often used for anesthesia induction |
| | |
| | |
|Ether |Obsolete |
| |Slow onset and recovery |
| |Post operative nausea, vomiting |
| |Low potency (must be combined with other agents to achieve anesthesia) |
|Nitrous Oxide |Rapid induction and recovery |
| |Both anesthetic and analgesic properties |
| |High potency anesthetic; combined w/ N2O |
| |No analgesic properties. |
|Haloethanes |Some hepatic metabolism occurs; repeated use causes hepatoxicity |
| |Also causes hypotension (thru vasodilation and cardiac suppression) |
| | |
| |High potency anesthetic; similar to haloethanes |
|Enfluran |Fewer side effects because less metabolized by liver. |
|Isofluran | |
|Desfluran | |
| |CNS – sedation, nausea, and cough suppression |
|Morphine |Respiratory System – reducing frequency and depth of breathing |
| |GI Tract – increases segmentation and decreases peristalsis (constipation) |
| |Eyes – papillary constriction (due to parasympathetic activation) |
|Codeine |Pro-drug, that is converted into morphine by CYP2D6. |
| |CYP2D6 inhibitors may reduce codeine efficacy, Genetic polymorphism may also explain |
| |codeine resistance |
| |Little euphoric effect, so low risk for addiction.Used as an anti-tussive (cough |
| |suppressant) |
| | |
| |Synthetic morphine derivative that does not act thru opioid receptors. |
|Dextromethrophan |Same efficacy as codeine |
| |No GI or analgesic effect |
|Heroin |Diamorphine; diacylated-morphine is more lipophilic than morphine so it crosses the |
| |blood-brain barrier more rapidly producing a greater rush. |
| |2x more potent than morphine |
|Hydrocodone | |
| | |
| |Vicodin; often combined w/ NSAIDs for synergistic effect |
| | |
| |Indicated for chronic pain. |
|Oxycodone |Addicts chew thru the slow release formulation to obtain immediate release to mimic |
| |heroin rush |
| | |
| |Similar to morphine, but shorter duration. |
|Meperidine |Used during labor. |
| |Similar to morphine, but much longer duration. |
| |Used to treat morphine/heroin addiction |
| | |
|Methadone | |
| |High potency. Can be used transdermally. |
| |Short-lasting. Used in anesthesia and patient controlled infusions. |
| | |
|Fentanyl | |
| | |
| |Opiate Antagonist |
|Naloxone |Short-acting competitive antagonist used to rapidly reverse opioid induced analgesia and|
| |respiratory suppression |
| | |
| |Opiate Antagonist |
|Naltrexone |Long-acting competitive antagonist |
| |Used to protect detoxified addicts from relapsing |
|Cocaine |-contains ester bond; rapidly metabolized by non-specific esterases in the plasma |
| |-cocaine’s CNS effects are independent from its analgesic effect |
| |(blocks reuptake of DA, 5-HT, NE) |
|Lidocaine |-contains amide bond; longer acting compared to local anesthetics w/ ester bonds |
|Classification of |Cell wall synth inhib |
|Antibiotics | |
| |Protein synth inhib |
| | |
| |Folate antagonists |
| | |
| |Quinolones |
|Penicillins | |
|Cephalosporins | |
|Carbapenems |All Beta-Lactam Antibiotics |
|Monbactams | |
|Vancomycin, Bacitracin | |
| |Penicillins, cell wall synth inhib |
|Benzylpenicillin |Inhibit transpeptidase, cant make cell wall |
| |Beta-lactamase sensitive |
|Phenoxymethylpenicillin |Narrow spectrum |
| |Phenoxy has better oral avail |
| |G+ bacteria |
| | |
|Methicillin |Narrow spectrum, b-lactamase resistant |
|Oxacillin |Cell wall synth inhib |
|Cloxacillin |G+ bacteria |
|Dicloxacillin |Methicillin=poor oral avail |
| |Oxacillin=good oral avail |
| | |
| | |
|Ampicillin |Broad spectrum, penicillinase sensitive |
| |Cell wall synth inhib |
|Amoxicillin |Amp=good oral avail, G+ and G-, entero |
| |Amox=excellent oral avail |
|Carbenicillin |Extended spectrum, b=lactamase sensitive, cell wall synth inhib |
|Ticarcillin |Carb=poor oral avail, G+ and G-, pseudomonas, Klebsiella |
|Mezlocillin | |
|Pipercillin | |
| | |
| |B-lactamase sensitive |
|Cefazolin |Cell wall synth inhib |
|Cephalexin |1st generation cephalorsporins |
| |Cross allergies with pen. |
| |G+ bacteria |
| | |
|Cefaclor |2nd generation Cephalosporins |
| |B-lactamase sensitive |
|Cefamandole |Cell wall synth inhib |
| |Some G-, mostly G+ |
|Cefoxitin | |
| | |
|Clavulanic Acid |B-lactamase inhib, cell wall synth inhib |
| |Irreversible inhib, good oral absorption |
|Sulbactam |Often combined with amoxicillin or ticarcillin |
| | |
|Vancomycin |Cell wall syth inhib |
| |Vanc=only effective against G+, poor oral absorption, used to treat GI infections |
|Bacitracin |Bacitracin=mixture of polypeptides, serious nephrotoxicity |
| | |
|Aminoglycosides |Protein synth inhib |
|Tetracyclins |Inhibit either 30s or 50s ribosomal unit |
|Macrolides |Drugs need to enter bacteria (point of resistance) |
|Chloramphenicol | |
|Clindamycin | |
|Gentamicin | |
|Tobramycin |Aminoglycosides (protein synth inhibitors) |
|Streptomycin | |
|Neomycin | |
|Kanamycin | |
|Amikacin | |
| |Tetracyclines, energy dependent transport, oral absorption impaired by food (antacids, |
| |Ca) |
|Tetracycline |Incorp into teeth and bones=staining, causes photosensitivity |
|Oxytetracycline |Broad spectrum antibiotics |
|Minocycline | |
|Doxycycline | |
| |Macrolides |
|Erythromycin |Narrow spectrum, good alternative for patients with allergy to pen, few side effects |
|Azithromycin |Azi=long T ½ , convenient 6 pills regimen |
|Clarithromycin |Clarith=used for H. pylori infection |
| |Protein synth inhib |
|Chloramphenicol |Chlor=broad spectrum, severe side effects, reserved for life threatening situations |
| |Clind=medium broad spectrum, treat pen resistant cocci |
|Clindamycin |Side effect=collitis |
|Sulfonamides | |
| |Folate antagonist, blocks folate synth=blocked replication |
|Sulfadiazine |Structural analogues of PABA |
|Sulfadimidine | |
|Sulfamethoxazole | |
| | |
|Trimethroprim |Competes with folates fro Dihydrofolate-reductase (folate antag), Similar to |
| |sulfonamides, combined with Sulfomethoxazole |
| |Treat UTIs |
| | |
| | |
|Quinolones |Inhibit DNA-Gyrase (Topoisomerase II), very broad spectrum, bactericidal, usually |
|Nalidixic acid |fluorinated |
|Ciprofloxacin |(Fluoroquinolones) |
|…floxacin | |
| | |
| | |
| | |
| | |
................
................
In order to avoid copyright disputes, this page is only a partial summary.
To fulfill the demand for quickly locating and searching documents.
It is intelligent file search solution for home and business.
Related download
- al al bayt university
- pharmacology basic principles
- type content here font arial size 12
- Ø 1e tool assessment of current antimicrobial stewardship
- routes of drug administration
- jhi paper structure by 5th march first draft 2nd july 2012
- northwestern medicine
- center for drug information and pharmacy practice1 abda