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TUBERCULOSIS CONTENTS: •INTRODUCTION •EPIDEMIOLOGY •CAUSES •PATHOGENESIS •DIAGNOSIS •TREATMENT • Tuberculosis or TB is a common and often deadly infectious disease caused by mycobacteria, usually Mycobacterium tuberculosis in humans. • Tuberculosis usually attacks the lungs but can also affect other parts of the body. • The classic symptoms are a chronic cough with blood-tinged sputum, fever, night sweats, and weight loss. CAUSES: • The primary cause of TB, Mycobacterium tuberculosis , is a small aerobic non-motile bacillus. • The M. tuberculosis complex includes four other TBcausing mycobacteria: M. bovis, M. africanum, M. canetti and M. microti. • M. africanum is not widespread, but in parts of Africa it is a significant cause of tuberculosis. EPIDEMIOLOGY: • It is currently estimated that 1/2 of the world's population (3.1 billion) is infected with Mycobacterium tuberculosis. Mycobacterium avium complex is associated with AIDS related TB. • The proportion of people who become sick with tuberculosis each year is stable or falling worldwide but, because of population growth, the absolute number of new cases is still increasing. • In 2007 there were an estimated 13.7 million chronic active cases, 9.3 million new cases, and 1.8 million deaths, mostly in developing countries. • The distribution of tuberculosis is not uniform across the globe; about 80% of the population in many Asian and African countries test positive in tuberculin tests, while only 5-10% of the US population test positive. Per 1,000,00 < 10 10 - 24 25 - 49 50 - 99 100 - 299 300 or more No estimate Highest estimated TB rates per capita were in Africa Transmission: • Pulmonary tuberculosis is a disease of respiratory transmission, Patients with the active disease (bacilli) expel them into the air by: • coughing, • sneezing, • shouting, • or any other way that will expel bacilli into the air Transmission is dependent on closeness and time of contact • Once inhaled by a tuberculin free person, the bacilli multiply 4 -6 weeks and spreads throughout the body. The bacilli implant in areas of high partial pressure of oxygen: • lung • renal cortex • reticuloendothelial system Signs and symptoms: • When the disease becomes active, 75% of the cases are pulmonary TB, that is, TB in the lungs. • Symptoms include chest pain, coughing up blood, and a productive, prolonged cough for more than three weeks. • Systemic symptoms include fever, chills, night sweats, appetite loss, weight loss, pallor, and often a tendency to fatigue very easily. Signs and symptoms: • In the other 25% of active cases, the infection moves from the lungs, causing other kinds of TB, collectively denoted extrapulmonary tuberculosis. This occurs more commonly in immunosuppressed persons and young children. • Extrapulmonary infection sites include the pleura in tuberculosis pleurisy, the central nervous system in meningitis, the lymphatic system in scrofula of the neck, the genitourinary system in urogenital tuberculosis, and bones and joints in Pott's disease of the spine. Pathophysiology Infection via inhalation of droplet nuclei. ↓ Transport of bacilli to terminal alveoli (especially lower segments of lungs) ↓ Ingestion of organisms by macrophages followed by multiplication within macrophages ↓ Transport of organisms to regional lymph nodes by infected macrophages with continue multiplication and minimal inflammatory response ↓ Extension of organisms( within 4-6 weeks after inhalation) into the bloodstream from the regional nodes ↓ Cell mediated immunity / hypersensitivity reaction ↓ Development of clinical infection Diagnosis by X-ray: Chest x-rays: Multi nodular infiltrate above or behind the clavicle with or without pleural effusion unilaterally or bilaterally. Diagnosis sputum investigation: • Cultures will reveal the presence of mycobacterium tuberculosis • Patients stay infectious for as long as the bacilli are excreted in the sputum Diagnosis by tuberculin test: Skin test. PPD (purified protein derivative) antigens are injected intradermally. A positive reaction is a helpful adjunct in diagnosis. Tuberculin test positivity indicated hypersentivity to bacterial protein Classification of drugs: According to their clinical utility the drugs are: • First line drugs : High antitubercular efficacy and low toxicity which are used routinely. • Second line drugs: Either low antitubercular efficacy or high toxicity or both, used in special circumstances only. First line drugs include: -ISONIAZIDE - PYRAZINAMIDE - ETHAMBUTOL -RIFAMPICIN -STREPTOMYCIN HIGH EFFICACY AND LOW TOXICITY Second line drugs include: -THIACETAZONE -CAPREOMYCIN -P-AMINOSALICYLIC ACID -ETHIONAMIDE -CYCLOSERINE -KANAMYCIN -AMIKACIN LOW EFFICACY AND HIGH TOXICITY NEWER SECOND LINE DRUGS: • Flouroquinolones are active against M.tuberculosis. Ciproflaxacin, Oflaxacin, • Newer macrolides and some rifampin congeners are the recent additions. Clarithromycin, Azithromycin, Rifabutin. Isoniazid (INH) (Isonicotinic acid hydrazide, H) • Primarily tuberculocidal • Tuberculocidal for rapidly multiplying bacilli • Acts on extracellular as well as on intracellular TB • Equally active in acidic or alkaline pH • One of the cheapest anti-tubercular drugs MECHANISM OF ACTION synthesizes Mycolic acids Isoniazid inhibits this synthesis Mechanism of Action Inhibition of synthesis of mycolic acids Two gene products labelled ‘InhA’ and ‘ KasA’ , which function in mycolic acid synthesis are targets of INH action INH enters sensitive mycobacteria which convert it by a catalaseperoxidase enzyme into a reactive metabolite then forms adduct with NAD that inhibits InhA and KasA INH enters bacilli by passive diffusion Drug is not directly toxic to the bacillus but must be activated to its toxic form within the bacillus by KatG (multifunctionary , catalase – peroxidase) KatG catalyzes the production from INH of an isoNicotinoyl radical that subsequently interacts with mycobacterial NAD and NADP to produce a dozen adducts A nicotinoyl-NAD isomer, inhibits the activities of enoyl acyl carrier protein reductase (InhA) and β-ketoacyl acyl carrier protein synthase (KasA) Inhibition of these enzymes inhibits synthesis of mycolic acid -- bacterial cell death Another Adduct, a nicotinoyl-NADP isomer , potently inhibits mycobacterial DHFRase ,thereby interfering with nucleic acid synthesis MOA of H: ISONIAZID Active INH AcpM & Kas Kat G( catalase peroxidase in mycobacteria) AcpM- Acyl Carrier protein KasA ( ß ketoAcyl Carrier protein synthetase) Block Mycolic Acid Synthesis Other products of KatG activation of INH include superoxide,H2O2 , alkyl hydroperoxides and NO radical may also contribute to INH bactericidal effect HOW DOES INH KILLS M. TUBERCULOSIS PRODURG ACTIVATED BY CATALYSE EANZYME PEROXYDASE (katG) UNABLE TO ENCODE ENOYL - ACP REDUCTASE OF FATTY ACID SYNTHASE II NO CONVERSION OF UNSATURATED FATTY ACIDS TO SATURATED FATTY ACIDS NO BIOSYNTHESIS OF MYCOLIC ACID M. TUBERCULOSIS CAN NOT SURVIVE PHARMACOKINETICS Absorption • Rapid and complete; rate can be slowed with food • Peak Plasma Time: 1-2 hr Distribution • All body tissues and fluids including CSF; crosses placenta; enters breast milk • Protein Bound: 10-15% Metabolism • Hepatic ( fast, slow acetylators) Elimination • Half-life elimination: fast acetylators: 30-100 min; slow acetylators: 2-5 hr; may be prolonged with hepatic or severe renal impairment • Excretion: Urine (75-95%); feces PHARMACOKINETICS Absorption • Rapid and complete; rate can be slowed with food • Peak Plasma Time: 1-2 hr Distribution • All body tissues and fluids including CSF; crosses placenta; enters breast milk • Protein Bound: 10-15% Metabolism • Hepatic ( fast, slow acetylators) Elimination • Half-life elimination: fast acetylators: 30-100 min; slow acetylators: 2-5 hr; may be prolonged with hepatic or severe renal impairment • Excretion: Urine (75-95%); feces Mechanism of resistance • Resistance can emerge rapidly if the drug is used alone. • Resistance can occur due to either 1. 2. High-level resistance is associated with deletion in the katG gene that codes for a catalase peroxidase involved in the bioactivation of INH. Low-level resistance occurs via deletions in the inhA gene that encodes “target enzyme” an acyl carrier protein reductase. Interactions with Isoniazid • Aluminium hydroxide inhibits INH absorption • INH retards phenytoin, carbamazepine, diazepam, theophylline and warfarin metabolism by inhibiting CYP2C19 and CYP3A4,and may raise their blood levels. • PAS inhibits INH metabolism and prologs its half life. Adverse effects of Isoniazid • Peripheral neuritis and a variety of neurological manifestations are the most important dose-dependent toxic effects. • INH neurotoxicity is treated by pyridoxine 100mg/day. • Hepatitis is major adverse effect of Isoniazid. • Lethargy • Rashes. • Fever acne. • Arthralgia. Adverse effects: • Hepatitis, a major adverse effect. • Respiratory syndrome: breathlessness. • Purpura, haemolysis, shock and renal failure. • Cutaneous syndrome : flushing, pruritis + rash. • Flu like syndrome : fever, headache, bone pain. Rifampin (Rifampicin , R) • Semisynthetic derivative of Rifamycin B obtained from streptomyces mediterranei • Bactericidal to M. Tuberculosis and many other gram(+) and gram (-) bacteria like staph.aureus , N.meningitidis, H.influenza, E.coli,Kleibsella , Pseudomonas,Proteus and legionella • Against TB bacilli , it is as efficacious as INH and better than all other drugs • Bactericidal actions covers all subpopulations of TB bacilli , but acts best on slowly or intermittenly dividing ones (spurters) • Both extra and intracellular organisms are affected • Good sterilizing and resistance preventing actions Mechanism of action of Rifampin • Rifampin interrupts RNA synthesis by binding to beta subunit of mycobacterial DNA-dependent RNA polymerase encoded by rpoB gene and blocking its polymerizing function • The basis of selective toxicity is that mammalian RNA polymerase does not avidly bind rifampin Mechanism of action • Interrupts RNA synthesis by binding to β subunit of mycobacterial DNA dependent RNA polymerase (encoded by rpoB gene ) MOA OF RIFAMPIN: D.N.A RIFAMPIN DNA dependent R.N.A.polymerase R.N.A Protein Syn. Cell multiplication Rifampin bind to β S.U of D.D.R.P Drug –Enz Complex Supression of chain initiation Rifampin resistance • Mycobacteria and other organisms develop resistance to rifampin rather rapidly. • Rifampin resistance is nearly always due to mutation in rpoB gene reducing its affinity for the drug. • No cross resistance with any other antitubercular drug,except rifampin congeners,has been noted. Pharmacokinetics • Well absorbed orally • Bioavailability ~ 70% , food decreases absorption • Rifampin is to be taken in empty stomach • Widely distributed in the body; • penetrates intracellularly , enters tubercular cavities, caseous masses and placenta • It crosses meninges , largely pumped out of CNS by P– glycoprotein • Metabolized in liver – active deacetylated metabolite – excreted mainly in Bile , some in urine • Rifampin and its deacetylated metabolite undergoes enterohepatic circulation • T1/2 – 2-5 hrs Interactions with rifampin •Rifampin is a microsomal enzyme inducer-increases severalCYP3A4, CYP2D6,CYP1A2 and CYP2C subfamily. •It thus enhances its own metabolism as well as that of many drugs including warfarin, oral contraceptives, corticosteroids, sulfonyl ureas, steroids, HIV protease inhibitors, non nucleoside reverse transcriptase inhibitors(NNRTIs), theophylline,metaprolol,fluconazol,ketoconazole, clarithromycin, phenytoin etc. •Contraceptive failures have occurred. •It is advisable to switch over to an oral contraceptive containing higher dose (50 microgram) of •Estrogen or use alternative method of contraception. Adverse effects of Rifampin oIncidence of adverse effects is similar to INH oHepatitis , a major adverse effect, generally occurs in pts with pre-existing liver disease and is dose related oJaundice – discontinuation of drug – reversible •Minor reactions, usually not requiring drug withdrawal and more common with intermittent regimens, are: oCutaneous syndrome: flushing, pruritus + rash (especially on face and scalp),redness and watering of eyes. oFlu syndrome: with chills ,fever, headache, malaise and bone pain. oAbdominal syndrome :nausea, vomiting, abdominal cramp with or without diarrhoea. Urine and secretions may become orange-red—but this is harmless. Other serious but rare reactions are: oRespiratory syndrome: breathlessness which may be associated with shock and collapse. oPurpura, haemolysis, shock and renal failure. Other uses of rifampin 1. 2. 3. 4. Leprosy Prophylaxis of Meningococcal and H.influenza meningitis and carrier state Second/third choice drug for MRSA, Diptheroids and legionella infections Combination of doxycycline and rifampin is first line therapy of brucellosis Pyrazinamide (Z) • Chemically similar to INH – Pyrazinamide was developed parallel to it (1952) • Weakly tuberculocidal • more active in acidic medium and slowly replicating bacteria • More lethal to intracellular bacilli and at sites showing inflammatory response • Highly effective during the first 2 months of therapy when inflammatory changes are present • Inclusion enabled duration of treatment to be shortened and risk of relapse to be reduced Mechanism of action of Pyrazinamide • not well established • Similar to INH – converted inside mycobacterial into active metabolite pyrazinoic acid by pyrazinamidase encoded by pncA gene • Gets accumulated in acidic medium and probably inhibits mycolic acid synthesis, but by interacting with a different fatty acid synthase • Pyrazinoic acid also appears to disrupt mycobacterial cell membrane and its transport function MOA OF PYRAZINAMIDE: • Pyrazinamide Mycobacterial Pyrazinamidase Pyrazinoic Acid Inhibits Mycolic Acid Synthesis PZA : MECHANISM OF ACTION PZA enter through passive diffusion Bac. Pyrazinamidase Pyrazinoic acid inhibit myobacterial fatty acid synthase -I INTERFERANCE IN CELL WALL SYSNTHESIS Pyrazinamide resistance •Resistance to Pyrazinamide develops rapidly if it is used alone and is mostly due to mutation in pncA gene. Pharmacokinetics of Pyrazinamide •Pyrazinamide is absorbed orally, widely distributed, has good penetration in CSF, because of which it is highly useful in meningeal TB; extensively metabolized in liver and excreted ion urine; plasma t½ is 6-10 hours. Adverse effects of Pyrazinamite • Hepatotoxicity is the most important dose-related adverse effect • Hyperuricaemia is common aid is due to inhibition of uric acid secretion in kidneys; gout can occur. • Other adverse effects are abdominal distress, arthralgia, flushing, rashes, fever and loss of diabetes control. Ethambutol (E) • Selectively Tuberculostatic • Active against MAC as well as some other mycobacteria • Fast multiplying bacilli – more susceptible • Added to triple regime of RHZ – hastens the rate of sputum conversion and prevents development of resistance Mechanism of action of Ethambutol • The mechanism of action of E is not fully understood, but it has been found to inhibit arabinosyl tranferases (encoded by embAB genes) involved in arabinogalactan synthesis thereby interfering with mycolic acid incorporation in mycobacterial cell wall. • Resistance to E develops slowly and is most commonly associated with mutation in embB gene, reducing the affinity of the target enzyme for E. • No cross resistance with any other antitubercular drug has been noted. ETHAMBUTOL : MECHANISM OF ACTION EXACT MECHANISM : NOT KNOWN PROBABILITIES : ETHAMBUTOL BLOCKS ARABINOSYL TRANSFERASE (ENCODED BY emb) NO POLYMERIZATION REACTION OF ARABINOGLYCAN INTERFERANCE IN CELL WALL SYSNTHESIS MOA OF E: Mycobact. Arabinosyl Transferase ETHAMBUTOL Polymerisation reaction of Arabinoglycan Essential component of Myco.Cellwall Pharamacokinetics of Ethambutol • About ¾ of an oral dose of E is absorbed. • It is distributed widely, but penetrates meninges incompletely and is temporarily stored in RBCs. • Less than½ of E is metabolized. • It is excreted in urine by glomerular filtration and tubular secretion; plasma t½ is ~4 hrs. • Caution is required in its use in patients with renal disease. Adverse effects of Ethambutol • Patient acceptability of E is very good and side effects are few. • Loss of visual acuity/colour vision, field defects due to optic neuritis is the most important dose and duration of therapy dependent toxicity. • With early recognition and stoppage of the drug, visual toxicity is largely reversible. • It is contraindicated in patients with optic neuritis. • Ethambutol produces few other symptoms: nausea, rashes, fever, rarely peripheral neuritis. • Hyperuricemia is due to interference with urate excretion. • It is safe during pregnancy. • Ethambutol is used in MAC infection as well Streptomycin • Streptomycin was isolated from a strain of Streptomyces griseus. • It was first clinically useful antitubercular drug. • It is aminoglycoside antibiotic. • It is tuberculocidal but less effective than INH or rifampin; acts only on extracellular bacilli. • Thus, other drugs and host defense mechanisms are needed to eradicate the disease. • It penetrates tubercular cavities,but does not cross CSF, and has poor action in acidic medium. • Limitation of its use i)dose related toxicity ii)development of resistant org. iii)pt compliance is poor due to i. m Streptomycin Mechanism of action: Irreversibly inhibits bacterial protein synthesis. Protein synthesis is inhibited in at least three ways: 1. Interference with the initiation complex of peptide formation. 2. Misreading of mRNA, which causes incorporation of incorrect aminoacids into the peptide, resulting in a nonfunctional or toxic protein. 3. Breakup of polysomes into nonfunctional monosomes. Streptomycin resistance •Resistance developed rapidly when streptomycin was used alone in tuberculosis-most patients had a relapse. •Recent studies indicate worldwide increase in resistance to streptomycin. •In case if streptomycin resistance infection, it must be stopped at the earliest because of risk of streptomycin dependence in which case the infection flourishes when the drug is continued. •Most nontubercular mycobacteria are unaffected by streptomycin. Pharmacokinetics • Absorption: IM: well absorbed; not absorbed from gut • Distribution: To extracellular fluid including serum, abscesses, ascitic, pericardial, pleural, synovial, lymphatic, & peritoneal fluids; crosses placenta; small amounts enter breast milk • Protein Bound: 34% • Half-life elimination: newborns: 4-10 hr; adults: 2-4.7 hr, prolonged with renal impairment • Excretion: urine (90% as unchanged drug); feces, saliva, sweat, & tears (<1%) SIDE EFFECTS: • OTOTOXICITY-drugs get conc. In labrynthine fluid, both vestibular & cochlear damage • NEPHROTOXICITY • PARALYSIS • Sterile abscess at the inj. site USE •Because of need for i.m. injections and lower margin of safety (ototoxicity and nephrotoxicity, especially in the elderly and those with impaired renal function) streptomycin is used only as an alternative to or in addition to other first line anti-TB drugs •Use is restricted to maximum of 2 months. •It is thus also labelled as a ‘supplemental’ first line drug. Second line drugs in TB • Less effective • More toxic • Used only if organism is resistant to first line drugs • Ethionamide , PAS, cycloserine : bacteriostatic • Amikacin, capromycin, fluoroquinolones are used in Multi Drug Resistant TB Second line drugs: • Aminoglycosides: least effective and more toxic Capreomycin - Viomycin – Kanamycin Adverse effects: • These drugs are: Nephrotoxic will cause Proteinuria, Hematuria, Nitrogen metabolism, and Electrolyte disturbances However effect is reversible when drug is stopped • Capreomycin has replaced viomycin because of less toxic effects, but all three drugs have the same effects. Cycloserine: • Can cause CNS disturbances • Therapeutic States : Cycloserine should be used when re-treatment is necessary or when the micro-organism is resistant to the other drugs. • It must be given in combination with other anti-tuberculosis drugs. • Dose: 500 mg to 1g per day • Mechanism of Action : An analog of D- alanine synthetase, will block bacterial cell wall synthesis. Thioacetazone & Ethionamide: • These are first anti tubercular drugs. • It is a tuberculostatic drug. • Low efficacy drug. • Side effects: hepatitis, optic neuritis, mental disturbences impotence Dose: 150mg per day Para-amino salicylic acid: • PAS is a tuberculostatic and one of least active drugs. • It inhibits denovo folate synthesis. • PAS is completely absorbed by oral route and distributed all over . • Dose : 150 mg/kg/day • Patient acceptability of PAS is poor. • Adverse effects ; Rashes, fever, liver dysfunction Chemotherapy DOTS: To control tuberculosis requires: • Effective, inexpensive, simple and standardised technology. The success of the DOTS strategy depends on: • Government commitment to a national tuberculosis programme. • Case detection –finding by smear microscopy examination of TB susceptible in general health services. • Regular uninterrupted supply of essential anti-TB drugs. • Monitoring system for programme supervised and evaluation. Short Course Chemotherapy: • These are regimens of 6-9 month duration. • All regimens have an initial intensive phase lasting 2-3 months to kill the TB bacilli and afford symptomatic relief. • This is followed by continuation phase for 4-6 months so that relapse does not occur. REGIMENS : Type of patient Duration of treatment Regimen Category-1 1.New sputum positive 2.Seriously ill, sputum negative, Pulmonary 3.Seriously ill Intensive phase(2months) INH+RMP+ETB+PZA Continuation phase(4months) INH+RMP Category-2 Retreatment group 1.Relapse 2.Treatment failure Intensive phase(3months) INH+RMP+ETB+PZA Continuation phase(5months) INH+RMP+ETB Category-3 1.New smear negative pulmonary 2.extrapulmonary Intensive phase(2months) INH+RMP+PZA Continuation phase(4months) INH+RMP Multiple Drug Resistance(MDR): • Resistance to both Isoniazid and Rifampin and number of other anti-TB drugs . MDR-TB has a more rapid course ,(some die in 4-16 weeks). • Treatment is difficult as second line drugs are less efficacious, less convenient, more expensive and toxic. • Therapy depends on drugs used in earlier regimen, dosage and regularity with which they have been taken. • In India>200,000patients have been treated under DOTS by early 2001 with cure rate of 75-80%. • In other countries 80-93%cure rates have been obtained. Chemotherapy Treatment of TB is categorised by: • Site of disease (pulmonary or extra pulmonary), its severity: the bacillary load and acute threat to life are taken into consideration. • Sputum smear positivity/negativity :positive cases are infectious. • History of previous treatment: risk of drug resistance is more in irregularly treated patients. SECOND LINE DRUGS Para amino salicylic acid Mechanism of action Aminosalicylic acid is a folate synthesis antagonist that is active almost exclusively against mycobacterium tuberculosis. It is structurally similar to p-amino benzoic acid(PABA) and the sulfonamides. Pharmacokinetics Absorption • T max is about 6 h Distribution • About 50% to 60% is protein bound. Elimination • 80% is excreted in the urine with at least 50% excreted in acetylated form. • The t 1/2 of free aminosalicylic acid is 26.4 min. Dose: 4g 3 times daily, children < 15yrs: 200-300mg/kg daily in 2-4 divided doses. Adverse Reactions GI • Nausea; vomiting; diarrhea; abdominal pain. Metabolic • Goiter with or without myxedema. Miscellaneous • Hypersensitivity (eg, fever, skin eruptions, leukopenia, thrombocytopenia, hemolytic anemia, jaundice, hepatitis, encephalopathy, Loffler syndrome, vasculitis). Drug Interactions Pregnancy • Category C . Lactation • Excreted in breast milk. Contraindications • Severe hypersensitivity to aminosalicylate sodium and its congeners. Precautions: Renal Function Impairment Drug and its acetyl metabolite may accumulate • Digoxin- May reduce oral absorption and serum levels of digoxin. • Rifampin- May decrease absorption of rifampin. • Vitamin B 12 May decrease GI absorption of oral vitaminB 12 . Hepatic Function- Use with caution. CHF • Use with caution because of high sodium content (55 mg of sodium per 500 mg tablet). Crystalluria • Maintain urine at neutral or alkaline pH to avoid crystalluria. Ethionamide Mechanism of Action: Ethionamide, like pyrazinamide, is a nicotinic acid derivative related to isoniazid. It is thought that ethionamide undergoes intracellular modification and acts in a similar fashion to isoniazid. Pharmacokinetics: • Absorption: completely absorbed following oral administration • Bioavailability approximately 100%. • Volume of distribution 93.5 L. • Protein binding :Approximately 30% bound to proteins. • Metabolism: Hepatic . Metabolized to the active metabolite sulfoxide, and several inactive metabolites. The sulfoxide metabolite has been demonstrated to have antimicrobial activity against Mycobacterium tuberculosis. • Route of elimination: Less than 1% of the oral dose is excreted as ethionamide in urine. • Half life2 to 3 hours Dose: Tuberculosis: • 15-20 mg/kg/day PO Max: 1000 mg/day Renal Impairment • CrCl <10 mL/min: decrease dose 50% Administration • Part of multi-drug regimen; not first-line treatment • Take with food Monitor: • baseline & periodic LFTs, TFTs, glucose Interactions Significant - Monitor Closely • cycloserine • isoniazid • magnesium oxide/anhydrous citric acid ADRS >10% • Disorder of gastrointestinal tract (50%) Frequency Not Defined • Postural hypotension • Dizziness • Drowsiness • Headache • Peripheral neuropathy • Psychosis Contraindications & Cautions Contraindications • Hypersensitivity to ethionamide • Severe hepatic dysfunction Cautions • Diabetes mellitus, thyroid disease, hepatic impairment Pregnancy & Lactation • Pregnancy Category: C • Lactation: excretion in milk unknown; use with caution CYCLOSERINE Cycloserine is an antibiotic produced by streptomyces orchidaceus. Mechanism of action : • It inhibits the incorporation of D- alanine into peptidoglycan pentapeptide by inhibiting alanine racemase, which converts Lalanine to D- alanine, and D- alanyl-D –alanine ligase (finally inhibits mycobacterial cell wall synthesis). • Cycloserine used exclusively to treat tuberculosis caused by mycobacterium tuberculosis resistant to first line agents Dosing and uses Active Tuberculosis • Initial: 250 mg PO BID • Maintenance: 500 mg -1 g/day in 2 divided doses for 18-24 months; not to exceed 1 g/day Renal Impairment • CrCl 50-80 mL/min: Give q12-16hr • CrCl 10-49 mL/min: Give q24-36hr • CrCl <10 mL/min: Contraindicated Administration • Part of multi-drug regimen; not first-line treatment Pharmacokinetics • Distribution: CSF concentration equal to that in plasma • Metabolism: liver • Excretion: urine INTERACTIONS Significant - Monitor Closely • ethionamide • isoniazid • magnesium oxide/anhydrous citric acid ADR Frequency Not Defined • Confusion • Dizziness • Headache • Somnolence • Seizure • Psychosis Contraindications & Cautions Contraindications • Hypersensitivity • Alcohol use • Renal dysfunction, severe • History of seizure disorder, mental depression, severe anxiety or psychosis Cautions • Alcoholism, anemia, impaired hepatic/renal function Pregnancy & Lactation • Pregnancy Category: C • Lactation: enters breast milk; safe Thioacetazone Mechanism of action: Bacteriostatic- inhibits cyclopropanaton of cell wall mycolic acids. Uses: It continues to be used as a convenient low cost drug to prevent emergence of isoniazid resistance, streptomycin & ethambutol. Dose:150mg OD in adults;2.5mg/kg in children; it is frequently combine with isoniazid T1/2: 12 hrs ADR: hepatitis, exfoliative dermatitis, SJS, bone marrow depression rarely Common: Abdominal discomfort, loose motions, rashes, mild anemia, anorexia. Azithromycin Mechanism of Action Binds to 50S ribosomal subunit of susceptible microorganisms and blocks dissociation of peptidyl t-RNA from ribosomes, causing RNA-dependent protein synthesis to arrest; does not affect nucleic acid synthesis Absorption • Rapidly absorbed • Bioavailability: 37%; variable effect with food • Peak plasma time: 2.3-4 hr Distribution • Extensively distributed into skin, lungs, sputum, tonsils, and cervix; penetrates cerebrospinal fluid (CSF) poorly • Protein bound: 7-50% (concentration dependent) • Vd: PO, 33.3 L/kg; IV, 31.1 L/kg Metabolism • Metabolized in liver Elimination • Half-life: Immediate release, ~70 hr; extended release, 59 hr • Excretion: Feces (50% as unchanged drug), urine (5-12%) Dose Mycobacterium Avium Complex Infection Prevention • 1.2 g PO once weekly; may be combined with rifabutin 300 mg once daily Treatment • 250 mg PO once daily in combination with ethambutol 25 mg/kg/day for 2 months 15 mg/kg/day plus rifabutin 300 mg/day or rifampin 600 mg/day Interactions Contraindicated • pimozide Serious - Use Alternative • BCG- vaccine live • Digoxin • Fondaparinux • heparin • Ondansetron • quinidine • typhoid vaccine live • warfarin ADRS >10%: Diarrhea (52.8%), Nausea (32.6%), Abdominal pain (27%), Loose stool (19.1%) 1-10%: Cramping (2-10%), Vaginitis (2-10%), Dyspepsia (9%), Flatulence (9%), Vomiting (6.7%), Malaise (1.1%) <1%: Agitation, Allergic reaction, Anemia, Anorexia, Candidiasis, Chest pain, Conjunctivitis, Constipation, Dermatitis (fungal), Dizziness, Eczema Contraindication • hypersensitivity • Cholestatic jaundice or hepatic impairment Cautions • Bacterial or fungal overgrowth may result from prolonged use • Prolonged QT interval: Cases of torsades de pointes have been reported. • Renal impairment (CrCl <10 mL/min) • Use with caution in patients with myasthenia gravis (exacerbation may occur) Administration IV Preparation • Dilute 500-mg vial in 4.8 mL of SWI (100 mg/mL) • Dilute further in NS to 1 mg/mL (500 mL) or 2 mg/mL (250 mL) IV Administration • 1 mg/mL solution: Infuse over 3 hours • 2 mg/mL solution: Infuse over 1 hour Pregnancy & Lactation • Pregnancy category: B • Lactation: Unknown whether drug is excreted into breast milk; use with caution Clarithromycin Mechanism of Action Semisynthetic macrolide antibiotic that reversibly binds to P site of 50S ribosomal subunit of susceptible organisms and may inhibit RNAdependent protein synthesis by stimulating dissociation of peptidyl tRNA from ribosomes, thereby inhibiting bacterial growth Pharmacokinetics • Absorption • Highly stable in presence of gastric acid (unlike erythromycin); food delays but does not affect extent of absorption • Bioavailability: 50% • Peak plasma time: 2-3 hr Distribution • Distributed widely into most body tissues except central nervous system (CNS) • Protein bound: 42-50% Metabolism • Partially metabolized by CYP3A4 • Metabolites: 14-OH clarithromycin (active) Elimination • Half-life: Immediate release, 3-7 hr; active metabolite, 5-9 hr • Renal clearance: Approximates normal glomerular filtration rate (GFR) • Excretion: Urine (30-55%) Dosing & Uses Mycobacterial Infection • Prophylaxis and treatment • 500 mg PO q12hr for 7-14 days Dosing Modifications • Renal impairment (CrCl <30 mL/min): Reduce normal dose by 50% ADR • >10%: Gastrointestinal (GI) effects, general (13%) • 1-10%: Abnormal taste (adults, 3-7%, Diarrhea (3-6%), Nausea (adults, 3-6%), Vomiting (adults, 1%; children, 6%), Elevated BUN; 4%, Abdominal pain (adults, 2%; children, 3%), Rash (children, 3%), Dyspepsia (2%), Headache (2%), Elevated prothrombin time (PT; 1%) • <1%: Anaphylaxis, Anxiety, Clostridium difficile colitis, Dizziness, Dyspnea, Elevated liver function tests Contraindications • hypersensitivity • Coadministration with pimozide, cisapride, ergotamine, and dihydroergotamine • History of cholestatic jaundice or hepatic dysfunction associated with previous use of clarithromycin • History of QT prolongation • Coadministration with HMG-CoA reductase inhibitors (statins) that are extensively metabolized by CYP3A4 (lovastatin, simvastatin), due to the increased risk of myopathy, including rhabdomyolysis Cautions • Severe renal impairment • Elderly patients may be more susceptible to drug-associated QT prolongation • Discontinue immediately if severe hypersensitivity reactions occur • Clostridium difficile associated diarrhea reported with use of nearly all antibacterial agents, including clarithromycin • Exacerbation of myasthenia gravis or new onset of symptoms reported Hepatic dysfunction • Increased liver enzyme activity and hepatocellular or cholestatic hepatitis, with or without jaundice, have been reported; this may be severe and is usually reversible Pregnancy & Lactation • Pregnancy category: C • Lactation: Drug is excreted in breast milk; use with caution AMIKACIN Mechanism of Action Irreversibly binds to 30S subunit of bacterial ribosomes; blocks recognition step in protein synthesis; causes growth inhibition. For gram-negative bacterial coverage of infections resistant to gentamicin and tobramycin Pharmacokinetics • Absorption: IM: May be delayed in bedridden patient • Vd: 0.25-0.4 L/kg, primarily into extracellular fluid (highly hydrophilic); penetrates blood-brain barrier when meninges inflamed; crosses placenta. • Excretion: urine (94-98%) • Half-Life: 2-3 hr • Peak Plasma Time: IM: 45-120 min • Protein Binding: 0-11% Dosing 15 mg/kg/day divided IV/IM q8-12hr Renal Impairment/Elderly • CrCl >90 mL/min & <60 years old: q8hr • CrCl 60-90 mL/min OR >60 years old: q12hr • CrCl 25-60 mL/min: q24hr • CrCl 10-25 mL/min: q48hr • CrCl <10 mL/min: q72hr Interactions Contraindicated • amphotericin b deoxycholate • cidofovir • neomycin Serious - Use Alternative • Atracurium • BCG- vaccine live • Bumetanide • cyclosporine • ethacrynic acid • Furosemide ADR • 1-10% • Neurotoxicity • Nephrotoxicity (if trough >10 mg/L) • Ototoxicity • <1%: Hypotension, Headache, Drug fever, Rash, Nausea, Vomiting, Eosinophilia, Tremor, Arthralgia Contraindications • Documented hypersensitivity Cautions • Renal impairment • Risk of neurotoxicity, ototoxicity, nephrotoxicity - risk of ototoxicity increase with concurrent loop diuretics Pregnancy & Lactation • Pregnancy Category: D • Lactation: excretion in milk unknown/not recommendedIV Preparation • Dilute 500 mg to 100 or 200 mL sterile diluent (usu NS or D5W) IV/IM Administration • IM: give undiluted to upper outer quadrant of buttocks • IV: infuse over 30-60 min in adults and children and 1-2 hr in infants KANAMYCIN Mechanism of Action Bactericidal and believed to inhibit protein synthesis by binding to 30 S ribosomal subunit. Pharmacokinetics •Metabolism: unknown •Excretion: urine Dosing & Uses • IV Administration: 5-7.5 mg/kg/dose divided q8-12hr; not to exceed 15 mg/kg/day divided q6-12hr; administer slowly • IM Administration: 5-7.5 mg/kg/dose divided q8-12hr; not to exceed 15 mg/kg/day IM divided q12hr at equally divided intervals; • Renal Impairment • CrCl 50-80 mL/min: give 60-90% of usual dose or give q8-12hr • CrCl 10-50 mL/min: give 30-70% of usual dose or give q12hr • CrCl <10 mL/min: give 20-30% of usual dose or give q24-48hr ADR Agranulocytosis, Anorexia, Diarrhea, Dyspnea, Elevated BUN, Enterocolitis, Headache, Incr salivation, Muscle cramps, Nausea, Nephrotoxicity, Neurotoxicity, Ototoxicity, Pruritus. Contraindications • Documented hypersensitivity Cautions • Auditory toxicity more common with kanamycin than with streptomycin and capreomycin; • monthly audiometry is recommended while patients are being treated with this drug; • renal toxicity occurs at a frequency similar to that of capreomycin; regular monitoring of serum creatinine recommended • Renal impairment • Myasthenia gravis • Nephrotoxic agents Pregnancy & Lactation • Pregnancy Category: D • Lactation: usually compatible ADMINISTRATION • IV Preparation • For adults, IV infusions are prepared by adding 500 mg of kanamycin to 100200 mL of usual IV infusion fluid such as NS or D5W or by adding 1 g of the drug to 200-400 mL of diluent • IV/IM Administration • Administer by deep IM injection, or IV infusion • May administer by intraperitoneal instillation, irrigation, or inhalation • Infuse over 30-60 min RIFABUTIN Mechanism of Action Inhibits DNA-dependent RNA polymerase Pharmacokinetics Absorption: readily, 53% Distribution: body tissues including the lungs, liver, spleen, eyes, & kidneys • Vd: 9.32 L/kg • Protein Bound: 85% • Bioavailability: absolute: HIV: 20% • Half-Life, 45 hr (range: 16-69 hr) • Peak Plasma Time: 2-4 hr Metabolism: hepatic CYP3A4 to active and inactive metabolites Excretion • Urine: 10% as unchanged drug, 53% as metabolites • Feces: 10% as unchanged drug, 30% as metabolites Prophylaxis • Indicated for prefention of disseminated Mycobacterium avium complex (MAC) disease in paitents with advanced HIV infection: 300 mg PO qDay • Patients with N/V diathesis: 150 mg PO BID with food Active TB (off-label) • 5 mg/kg PO qD or 2-3x/week + other antitubercular agents, no more than 300 mg/dose Renal Impairment • CrCl<30mL/min dose should be reduced by 50% Interactions • artemether • Clarithromycin ADR: >10%: Discoloration of urine (30%), Neutropenia (25%), Leukopenia (17%), Rash (11%) 1-10%: Incr AST/ALT (7-9%), Thrombocytopenia (5%), Abdominal pain (4%), Diarrhea (3%), Eructation (3%), Headache (3%), Nausea/vomiting (3%), Anorexia (2%), Flatulence (2%) Contraindications & Cautions Contraindications • Hypersensitivity to rifamycins • Concomitant live bacterial vaccines Cautions • Monitor hematologic status • Eye pain, redness, loss of vision may indicate inflammatory ocular condition • May have brown-orange color of urine, feces, saliva, sputum, perspiration, tears, & skin • Pregnancy Category: B Fluoroquinolones Ciprofloxacin, Levofloxacin, gatifloxacin, moxifloxacin can inhibit strains M tuberculosis. They are also active against atypical mycobacteria. Moxifloxacin is the most active against M tuberculosis. Mechanism of action: They inhibit bacterial DNA synthesis by inhibiting bacterial topoisomerase II (DNA Gyrase) and topoisomerase IV. • Inhibition of DNA Gyrase prevents the relaxation of supercoiled DNA that is required for normal transcription and replication. • Inhibition of topoisomerase IV interferes with separation of replicated chromosomal DNA into the daughter cells during cell division. Pharmacokinetics Rapidly absorbed orally- but food delays absorption, BA: C- 60-80%, L- 100%, G- 96% PPB: C- 20-35%, L- 15%, G- 20% Vd: C- 3-4%, L-8%, Half life: C- 3-5hrs, L-8hrs, G- 8hrs High tissue penetration: lungs, sputum, muscle, prostate but low in CSF Excreted primarily in urine, urinary and biliary concentrations are 10-50 times more than plasma Ciprofloxacin 750mg BD,PO Levofloxacin 500mg OD.PO Moxifloxacin 400mg OD. PO Dosage Adverse effects Nausea, vomiting,diarrhoea(most common). Headache, dizziness, insomnia, skin rash, photosensitivity. Damage growing cartilage and cause an arthropathy. Tendinitis, tendon rupture. Interactions • All fluoroquinolones interact with aluminum- or magnesium-containing antacids and products containing calcium, iron, or zinc. Concomitant use invariably results in marked reduction of oral absorption of the antimicrobial and decreased the bioavailability of these drugs by up to 98% when given within 2 hours of antibiotic administration. • Fluoroquinolones are administered with food, peak concentration times are usually slightly delayed, and maximum plasma concentrations (Cmax) are decreased 8-16%. • Reductions in renal and total systemic clearance caused by probenecid are 24% for levofloxacin,[50% for ciprofloxacin, and 42% for gatifloxacin. • Significantly interact with theophylline-ciprofloxacin decreased theophylline clearance by 25-30%, and increased theophylline plasma concentrations by up to 308%. THANK YOU -PHARMA STREET