SlideShare a Scribd company logo

Everything You Need to Know About Quinolones

Download as PPTX, PDF
S
Shubham Marbade

Quinolones and fluoroquinolones are a class of broad-spectrum antibacterial drugs. They work by inhibiting bacterial DNA gyrase and topoisomerase enzymes. While quinolones like nalidixic acid were the first discovered, fluoroquinolones like ciprofloxacin are more potent and have a broader range of activity. Fluoroquinolones are widely used to treat urinary tract, respiratory, gastrointestinal, skin and soft tissue infections. Adverse effects can include gastrointestinal issues and central nervous system effects. Their use is contraindicated in some groups like pregnant women and children. Some fluoroquinolones are being investigated for repurposing as anticancer agents and for

Science
1 of 41
QUINOLONES By Shubham Marbade M.Pharm Pharmacology
Quinolones • Synthetic, broad spectrum and bactericidal. • Effective after oral administration for wide variety of infectious diseases, • Play an increasingly important role in treatment of multi-drug resistant bacterial infections. • They are widely used because of their relative safety, availability both orally & parenterally and their favorable pharmacokinetics.
• Nalidixic acid was the first quinolone discovered in 1960s and primarily used for urinary tract infection.
Fluoroquinolones • Wide variety of application and broad spectrum antibiotic • More potent than quinolones. • Modified quinolones with one or more fluorine atom in their structure.
Classification
PHARMACOKINETIC • Rapidly and almost completely absorbed after oral administration and are widely distributed in body tissues. • Peak serum levels are obtained within 1- 3 hours of an oral dose of 400mg with peak levels ranging from 1.1 ug/ ml for sparfloxacin to 6.4 ug/ml for levofloxacin . • Food does not impair oral absorption but may delay. • Bioavailability is > 50% for all agents and > 95% for several.
• Half life s 3- 5 hours for norfloxacin and ciprofloxacin. • The volume of distribution of quinolones is high with concentration of quinolones n urine, kidney, lung, and prostate tissue, stool, bile and macrophage and neutrophils higher than serum levels. • Concentration in CSF, bone and Prostatic fluid are lower than in serum. • The fluoroquinolones are also metabolized by hepatic conjugation and glucuronidation. Dosage, peak serum levels, percent protein binding, urine concentrations, and degree of metabolism differ to varying degrees among the quinolones.
• It is excreted primarily in urine, both by glomerular filtration and tubular secretion. • Urinary and biliary concentrations are 10–50 fold higher than plasma.
Mechanism of action • These agents targets DNA gyrase and Topoisomerase IV. • For Gram – ve bacteria DNA gyrase, and for Gram + ve bacteria topoisomerase IV is primary site for their activity. • These drugs binds to A- subunit of DNA gyrases and four subunits of topoisomerase IV enzyme which are responsible for unwinding of supercoiled DNA for process of replication and transcription. • Thus it results in blockade of unwinding and inhibition of replication. • Synthesis of protein inhibited. • inhibition of growth of bacteria and kills bacteria.
Antibacterial spectrum • Quinolones have broad spectrum antibacterial activity against various Gram +ve and Gram -ve bacterias including E. coli, Salmonella, Sheigella, P. aeruginosa, Clamydia, mycoplasma, Brucella, Mycobacterium, legionella etc.
Antibacterial Resistance • Resistance to the quinolones develops due to mutation to bacterial chromosomal genes of Gyrase A and Topoisomerase IV encoding information to unwind Supercoiled DNA. • No quinolone modifying or inactivating activity has been seen to develop resistance.
Therapeutic Uses 1. Urinary tract infections: High cure rates, even in complicated cases or those with indwelling catheters/prostatitis, have been achieved. ChronicPseudomonas infections respond less completely. 2. Gonorrhoea: Initially a single 500 mg dose was nearly 100% curative in non-PPNG as well as PPNG infections, but cure rate has declined in the recent years due to emergence of resistance. 3. Chancroid: 500 mg BD for 3 days is an excellent alternative to ceftriaxone/erythromycin. 4. Bacterial gastroenteritis: Severe cases due toEPEC, Shigella, Salmonella and Campy. jejunirespond quickly. It has also been used to reducestool volume in cholera.
5. Typhoid: Ciprofloxacin is the first choice drug in typhoid fever since chloramphenicol, ampicillin and cotrimoxazole have become unreliable due to development of resistance. A dose of 500–750 mg BD for 10 days is recommended. Patients unable to take the drug orally may be treated with 200 mg. i.v. 12 hourly in the beginning. 6. Bone, soft tissue, gynaecological and wound infections: caused by resistant Staph. and gramnegative bacteria: high cure rates have been obtained but prolonged treatment with high doses is required in osteomyelitis and joint infections.Used along with clindamycin/ metronidazole (to cover anaerobes) it is a good drug for diabetic foot.
7.Respiratory infections: Ciprofloxacin can treat Mycoplasma,, H. influenzae, Branh. catarrhalis and some streptococcal and pneumococcal infections besides gram-negative ones. 8.Tuberculosis It is now frequently used as acomponent of combination chemotherapy against multidrug resistant tuberculosis. Recently, even FQ-resistant TB have arisen. 9.Gram-negative septicaemias: Parenteral ciprofloxacin may be combined with a third generation cephalosporin or an aminoglycoside.
• 10. Meningitis: Though penetration in CSF is not very good, ciprofloxacin has been successfully used in gram-negative bacterial meningitis, especially that occurring in immunocompromised patients or those with CSF shunts.
Adverse Effects • GI tract- (2–13%) these include nausea, vomiting, diarrhea, and abdominal pain. • CNS effects- (1–8%) such as drowsiness, weakness, headache, dizziness, and in severe cases, convulsions and toxic psychosis, have been reported. • sparfloxacin and lomefloxacinv shows photosensitivity included second-degree burns, discoloration and sometimes permanent discoloration and scarring of the skin due to halogen substitution on the eighth position, as found in
• Adverse cardiovascular effects (6–7%; vascular embolism, cardiac insufficiency, hypotension) also occur with sparfloxacin. Sparfloxacin, moxifloxacin, and gatifloxacin can exacerbate QT prolongations. • Fulminant hepatotoxicity associated withtrovafloxacin has resulted in acute liver failure, and the FDA has recommended limiting therapy to life-threateninginfections.
• Allergic reactions (e.g., rashes, urticaria, and eosinophilia) have been observed. These drugs have occasionally been associated with cholestatic jaundice, blood dyscrasias, hemolytic anemia, hypoglycemia, and nephrotoxicity. • Recently the use of ciprofloxacin for prophylaxis protection against anthrax infection has been associated with damage to muscle ligaments.
Drug Interactions • All quinolones interact with multivalent cations, forming chelation complexes resulting in reduced absorption. • Major offenders are antacids; vitamins containing calcium and iron can also be problematic. All fluoroquinolones interact with warfarin, didanosine, and phenytoin, resulting in decreased absorption or metabolism. • Ciprofloxacin and other second-generation drugs interact with theophylline by decreasing its clearance, which leads to theophylline toxicity.
Contraindications • The use of the quinolones in pregnant or breastfeeding women and children whose epiphysial plates have not closed is generally contraindicated. • Their use for treating young cystic fibrosis children infected with Pseudomonas species is an exception; the patient should be monitored carefully for untoward effects.
• These drugs contraindicated in arrhythmia because it prolong the heart's QT internal by blocking voltage-gated potassium channels lead to a life-threatening arrhythmia.
Nalidixic acid • It is active against gram-negative bacteria, especially E. coli, Proteus, Klebsiella, Enterobacter, Shigella but not Pseudomonas. It acts by inhibiting bacterial DNA gyrase and isbactericidal. • Absorbed orally, highly plasma protein bound and partly metabolized in liver. It is excreted in urine with a plasma t½ ~8 hrs. • Concentration of the free drug in plasma and most tissues attained with the usual doses is non therapeutic • for systemic infections. • Dose: 0.5–1 g TDS or QID
Ciprofloxacin • It is the most potent first generation FQ active against a broad range of bacteria, the most susceptible ones are the aerobic gram-negative bacilli, especially the Enterobacteriaceae and Neisseria. • It binds to divalents cations which decreases absorption. • Because of its good penetration into bone, orally administered ciprofloxacin is a useful alternative to parenterally administered antibiotics for the treatment of osteomyelitis caused by susceptible organisms. • Dose- 250, 500, 750 mg tab, 200 mg/100 ml i.v. infusion, 3 mg/ml eye drops.
Levofloxacin • It is the levoisomer of ofloxacin having improved activity against Strep. Pneumoniae and some other gram-positive and gramnegative bacteria. • Oral bioavailability of levofloxacin is nearly 100%; oral and i.v. doses are similar. • The primary indication of levofloxacin is community acquired pneumonia and exacerbations of chronic bronchitis in which 87–96% cure rate has been obtained. • High cure rates have been noted in sinusitis, enteric fevers, pyelonephritis and skin/soft tissue infections as well. • Dose- 500 mg tab, 500 mg/100 ml inj.
Trovafloxacin • Trovafloxacin is a broad spectrum antibiotic inhibit the uncoiling of supercoiled DNA in various bacteria by blocking the activity of DNA gyrase and topoisomerase IV. • It was shown to be more effective against Gram- positive bacteria than Gram-negative bacteria when compared to previous fluoroquinolones. • Gonorrhea in males and endocervical and rectal gonorrhea in females as well as non gonoccocal urethritis and cervicitis. • Well-absorbed from the gastrointestinal tract after oral administration and does not depend on concomitant food intake. The absolute bioavailability is approximately 88%. • Dose- 300 mg iv and 100 mg tid
Repositioning to Anticancer agents • Several FQs just like anyother anticancer drug have been shown to cause cell cycle arrest primarily in S and G2phase of progression. • Several studies reveals the ability of ciprofloxacin to induce S/G2-phase arrest in bladder and prostate cancer cells. Similarly, enoxacin revealed its ability to induce S/G2-phase in prostate cancer cells and G2/M-phase arrest in breast cancer cells. • Later on, few more studies showed similar S/G2-phase arresting effects of other FQs like lomefloxacin, ofloxacin and levofloxacin in epidermoid carcinoma and breast cancer cells respectively. • Ciprofloxacin possesses the maximum efficacy in inducing apoptosis. It shows potent anti-proliferative effect to induce apoptosis in bladder cancer cells and then later on in prostate cancer cells.
Clinafloxacin • Methicillin resistant Staphylococcus aureus (MRSA) has developed numerous mechanisms of virulence and strategies to evade the human immune system which are difficult to treat infections in human beings, and becoming important cause of morbidity and mortality. • Acts as novel inhibitors of bacterial efflux pump, FtsZ, DNA gyrase, and topoisomerase IV and have the potential to exert multiple mechanisms of action.
Fluoroquinolones in treatment of TB • Fluoroquinolones like moxifloxacin, gatifloxacin and levofloxacin, are the most valuable second- line anti-TB agents according to the current WHO guidelines. • These drugs are currently under clinical trial for pulmonary tuberculosis and tuberculosis meningitis. • The aim of this study is to provide an alternative to resistant drug to prevent failure of treatment and emergence of drug resistance.
Delafloxacin in ABSSSI • Delafloxacin is a novel anionic fluoroquinolone (FQ) approved for treatment of acute bacterial skin and skin structure infections (ABSSSIs) caused by a number of Gram-positive and Gram-negative organisms including MRSA and Pseudomonas aeruginosa. • It is more potent than other quinolones against Gram +ve bacteria and Gram –ve bacteria. • It is considered a dual-targeting FQ and displays nearly equivalent affinity for DNA gyrase and topoisomerase IV. • This property likely explains delafloxacin’s broad spectrum of in vitro activity against both GN and GP bacteria
Delafloxacin in CABP • Approved for use in adults for the treatment of community-acquired bacterial pneumonia, delafloxacin was shown in a phase III clinical trial to be superior to moxifloxacin in patients with CABP who also have chronic obstructive pulmonary disease (COPD) or asthma as a comorbidity, and in CAP patients who may have severe illness. • Additionally, delafloxacin appeared to be better tolerated compared to commonly used FQs.
Levonadifloxacin • It is a novel antibacterial agent belonging to benzoquinolizine subclass of fluoroquinolones which is under clinical development as a parenteral formulation and its prodrug alalevonadifloxacin as an oral option. Both the drugs have been approved recently in India based on phase III trial completed for ABSSSI.
Fluoroquinolones in catheter coating • Antimicrobial catheter coatings were prepared by immobilizing fluoroquinolones either with the use of linkers (covalent binding) or by activating the polymer matrix with iodine/bromine (noncovalent binding). • The new antimicrobial coatings, obtained with the participation of fluoroquinolone antibiotics in an uncomplicated way, are able to protect the urinary catheters against bacterial infections during catheterization. • Since the ideal antibacterial material has not yet been found, there is still a need to look for new ways of the prevention of catheter- associated urinary tract infections
Sparfloxacin • Ocular diseases affect a growing number of people across the globe. Some pathological ophthalmic conditions, such as glaucoma, diabetic retinopathy, or age-related macular degeneration, cause severe visual impairment that can ultimately lead to blindness. • Nanosuspensions were prepared via a solvent diffusion technique and loaded with sparfloxacin used against bacterial conjunctivitis. • The optimal formulation was the one based on N- carboxymethyl CS nanosuspension in combination with sustainable sparfloxacin release.
Antifungal activity • Quinolones and Flouroquinolones displayed potential anti-fungal activity and some of them could significantly increase the susceptibility of antifungals. • Metal complexes of Flouroquinolones with specified antimicrobial activities, are a new entry in the field of bioinorganic. • Zone of inhibition values of fluoroquinolones are compared with parent drug. • Some of them found to exhibit excellent potency against both drug‐susceptible and drug‐resistant fungi where as some found to show lesser or no antifungal behavior as compared to the parent drug.
Bioprinting Technology • liver bioengineering has picked up momentum in recent years for the development of both artificial substitutes for supporting repair/regeneration as well as in vitro hepatic models for clinical and diagnostic application. • Trovafloxacin is used to induce liver txicity at tissue level. • Compared to conventional 2D models, trovafloxacin treatment resulted in significant, dose-dependent toxicity at clinically relevant doses (≤4 μM) in the developed 3D models.
Sitafloxacin • According to study carried out in Japan : Sitafloxacin based therapy is a potent candidate for third-line Helicobacter pylori eradication treatment. • The 7-day regimen with vonoprazan 20 mg b.i.d., sitafloxacin 100 mg b.i.d., and amoxicillin 750 mg b.i.d. or 500 mg q.i.d. is a good option as the third-line H. pylori eradication treatment
Immunomodulatory Effects of Fluoroquinolones • Immune responses are indirectly modulated by FQs through suppressing pro-inflammatory cytokines, such as interleukin 1 (IL-1), IL-6, tumor necrosis factor-alpha (TNF-α), and super-inducing IL-2, which tend to increase both the growth and activity of T and B lymphocytes. In addition, they affect the development of immune responses by influencing of expression of other cytokines and mediators.
References • Yadav V, Talwar P, Repositioning of fluoroquinolones from antibiotic to anti-cancer agents: Anunderestimated truth, Biomedicine and pharmacotherapy, 2019, 111, 934- 946. • Xuemei Ge, Zhi Xu, 1,2,4-Triazole hybrids with potential antibacterial activity against methicillin resistant Staphylococcus aureus, Arch Pharm DPhG, 2020, 1- 10. • Dorota Kowalczuk et al, FTIR Characterization of the Development of Antimicrobial Catheter Coatings Loaded with Fluoroquinolones, coating, 2020, 10, 818 • Alexandra Zamboulis et al, Chitosan and its Derivatives for Ocular Delivery Formulations: Recent Advances and Developments, Polymers, 2020, 12, 1519 • Savita Khatria, Manoj Kumara, Pratibha, Rajesh Kumar, A Review of Antifungal Activities of Various Flouroquinolone and Its Metal Complexes, annals of R S C B 2021, 21(5 ), 396- 405 • Tarun Agarwal et al., Recent advances in bioprinting technologies for engineering hepatic tissue, Materials Science & Engineering C, 2021, 123 • Toshihiro Nishizawa et al, Sitafloxacin for Third-Line Helicobacter pylori Eradication: A Systematic Review, J. Clin. Med. 2021, 10, 2722.
• Shokrollah Assar et al, A Review of Immunomodulatory Effects of Fluoroquinolones, A Journal of Molecular and Cellular Immunology, 2020 • Pranger AD et al, The Role of fluoroquinolones of in the treatment of tuberculosis 2019, Cross Mark, 2019, 79, 161- 171. • Sharma R, et al, Community Acquired Bacterial Pneumonia- Changing Epidemiology, Resistance Patterns and Newer Antibiotics: Spotlight n Delafloxacin, Clinical drug Investigation, 2020, 40, 947- 960. • Chabner B, Knollman B, Goodman and Gilman’s The Pharmacological Basis of Therapeutics, 12th Edition, 1470 • Tripathi KD, Essentials of Medical Pharmacology, 6th edition, Jaypee Brothers Medical Publishers, 2003, 687. • Craig CR, Stitzel RE, Modern Pharmacology with Clinical Application, 5th Edition, 519.

Recommended

Quinolones & Fluoroquinolones
Quinolones & FluoroquinolonesQuinolones & Fluoroquinolones
Quinolones & FluoroquinolonesDr Resu Neha Reddy
 
Serotonin
SerotoninSerotonin
SerotoninRaghavendra institute of pharmaceutical education and research .
 
Macrolide antibiotics
Macrolide antibioticsMacrolide antibiotics
Macrolide antibioticsDr Vinay Gupta
 
Aminoglycoside by sumit
Aminoglycoside by sumitAminoglycoside by sumit
Aminoglycoside by sumitSumit Kumar
 
Macrolide antibiotics
Macrolide antibioticsMacrolide antibiotics
Macrolide antibioticsandhra university
 
Anti-Hyperlipidemic Drugs (Pharmacology -II) By- Anshik Srivastava.pdf
Anti-Hyperlipidemic Drugs (Pharmacology -II) By- Anshik Srivastava.pdfAnti-Hyperlipidemic Drugs (Pharmacology -II) By- Anshik Srivastava.pdf
Anti-Hyperlipidemic Drugs (Pharmacology -II) By- Anshik Srivastava.pdfSanskriti College of Higher Education and Studies
 
Pro-Kinetic Agents
Pro-Kinetic AgentsPro-Kinetic Agents
Pro-Kinetic AgentsKhalid Ghaznavi
 
Quinolones and fluoroquinolones
Quinolones and fluoroquinolonesQuinolones and fluoroquinolones
Quinolones and fluoroquinolonesKoppala RVS Chaitanya
 

Recommended

Quinolones & Fluoroquinolones
Quinolones & FluoroquinolonesQuinolones & Fluoroquinolones
Quinolones & FluoroquinolonesDr Resu Neha Reddy
 
Serotonin
SerotoninSerotonin
SerotoninRaghavendra institute of pharmaceutical education and research .
 
Macrolide antibiotics
Macrolide antibioticsMacrolide antibiotics
Macrolide antibioticsDr Vinay Gupta
 
Aminoglycoside by sumit
Aminoglycoside by sumitAminoglycoside by sumit
Aminoglycoside by sumitSumit Kumar
 
Macrolide antibiotics
Macrolide antibioticsMacrolide antibiotics
Macrolide antibioticsandhra university
 
Anti-Hyperlipidemic Drugs (Pharmacology -II) By- Anshik Srivastava.pdf
Anti-Hyperlipidemic Drugs (Pharmacology -II) By- Anshik Srivastava.pdfAnti-Hyperlipidemic Drugs (Pharmacology -II) By- Anshik Srivastava.pdf
Anti-Hyperlipidemic Drugs (Pharmacology -II) By- Anshik Srivastava.pdfSanskriti College of Higher Education and Studies
 
Pro-Kinetic Agents
Pro-Kinetic AgentsPro-Kinetic Agents
Pro-Kinetic AgentsKhalid Ghaznavi
 
Quinolones and fluoroquinolones
Quinolones and fluoroquinolonesQuinolones and fluoroquinolones
Quinolones and fluoroquinolonesKoppala RVS Chaitanya
 
Sexually transmitted infections
Sexually transmitted infectionsSexually transmitted infections
Sexually transmitted infectionsPravin Prasad
 
Macrolide (l)
Macrolide (l)Macrolide (l)
Macrolide (l)Rahul Kunkulol
 
Antiulcer
AntiulcerAntiulcer
AntiulcerMonika Verma
 
Anti histamines-1.pptx
Anti histamines-1.pptxAnti histamines-1.pptx
Anti histamines-1.pptxABDULRAUF411
 
Penicillins
PenicillinsPenicillins
PenicillinsNarasimha Kumar G V
 
pharmacology of Rheumatoid arthritis
pharmacology of Rheumatoid arthritis pharmacology of Rheumatoid arthritis
pharmacology of Rheumatoid arthritis Mohd Asad Farooqui
 
Antiemetics
AntiemeticsAntiemetics
AntiemeticsMayur Chaudhari
 
Anti diarrhoeals & laxative
Anti diarrhoeals & laxativeAnti diarrhoeals & laxative
Anti diarrhoeals & laxativeRahul B S
 
Antibiotics chloramphenicol and macrolides
Antibiotics chloramphenicol and macrolidesAntibiotics chloramphenicol and macrolides
Antibiotics chloramphenicol and macrolidesGrace Felciya
 
Drug acting on inflammatory bowel disease
Drug acting on inflammatory bowel diseaseDrug acting on inflammatory bowel disease
Drug acting on inflammatory bowel diseaseAlisha Talwar
 
Antiamoebic drugs
Antiamoebic drugsAntiamoebic drugs
Antiamoebic drugsBhudev Global
 
Drugs Used in Urinary Tract Infection
Drugs Used in Urinary Tract InfectionDrugs Used in Urinary Tract Infection
Drugs Used in Urinary Tract InfectionPravin Prasad
 
Serotonin
SerotoninSerotonin
SerotoninDr. Rupendra Bharti
 
peptic ulcer & their new molecular target
peptic ulcer & their new molecular targetpeptic ulcer & their new molecular target
peptic ulcer & their new molecular targetKundlik Rathod
 
Plecanatide
PlecanatidePlecanatide
PlecanatideDr Nikita Ingale
 
proton pump inhibitors PPT
proton pump inhibitors PPTproton pump inhibitors PPT
proton pump inhibitors PPTpharmastuffblogspotcom
 
Macrolides
MacrolidesMacrolides
MacrolidesAminu Kende
 
Anti emetics
Anti emeticsAnti emetics
Anti emeticsMerin Babu
 
Anti ulcer, anti-emetic and prokinetics
Anti ulcer, anti-emetic and prokineticsAnti ulcer, anti-emetic and prokinetics
Anti ulcer, anti-emetic and prokineticsGamitKinjal
 
Prokinetics
ProkineticsProkinetics
ProkineticsTehran University of Medical Sciences
 
Quinolones.pptx
Quinolones.pptxQuinolones.pptx
Quinolones.pptxSubramani Parasuraman
 
Quinolones
QuinolonesQuinolones
QuinolonesJagirPatel3
 

More Related Content

What's hot

Sexually transmitted infections
Sexually transmitted infectionsSexually transmitted infections
Sexually transmitted infectionsPravin Prasad
 
Anti histamines-1.pptx
Anti histamines-1.pptxAnti histamines-1.pptx
Anti histamines-1.pptxABDULRAUF411
 
pharmacology of Rheumatoid arthritis
pharmacology of Rheumatoid arthritis pharmacology of Rheumatoid arthritis
pharmacology of Rheumatoid arthritis Mohd Asad Farooqui
 
Anti diarrhoeals & laxative
Anti diarrhoeals & laxativeAnti diarrhoeals & laxative
Anti diarrhoeals & laxativeRahul B S
 
Antibiotics chloramphenicol and macrolides
Antibiotics chloramphenicol and macrolidesAntibiotics chloramphenicol and macrolides
Antibiotics chloramphenicol and macrolidesGrace Felciya
 
Drug acting on inflammatory bowel disease
Drug acting on inflammatory bowel diseaseDrug acting on inflammatory bowel disease
Drug acting on inflammatory bowel diseaseAlisha Talwar
 
Drugs Used in Urinary Tract Infection
Drugs Used in Urinary Tract InfectionDrugs Used in Urinary Tract Infection
Drugs Used in Urinary Tract InfectionPravin Prasad
 
peptic ulcer & their new molecular target
peptic ulcer & their new molecular targetpeptic ulcer & their new molecular target
peptic ulcer & their new molecular targetKundlik Rathod
 
Anti ulcer, anti-emetic and prokinetics
Anti ulcer, anti-emetic and prokineticsAnti ulcer, anti-emetic and prokinetics
Anti ulcer, anti-emetic and prokineticsGamitKinjal
 

What's hot (20)

Sexually transmitted infections
Sexually transmitted infectionsSexually transmitted infections
Sexually transmitted infections
 
Macrolide (l)
Macrolide (l)Macrolide (l)
Macrolide (l)
 
Antiulcer
AntiulcerAntiulcer
Antiulcer
 
Anti histamines-1.pptx
Anti histamines-1.pptxAnti histamines-1.pptx
Anti histamines-1.pptx
 
Penicillins
PenicillinsPenicillins
Penicillins
 
pharmacology of Rheumatoid arthritis
pharmacology of Rheumatoid arthritis pharmacology of Rheumatoid arthritis
pharmacology of Rheumatoid arthritis
 
Antiemetics
AntiemeticsAntiemetics
Antiemetics
 
Anti diarrhoeals & laxative
Anti diarrhoeals & laxativeAnti diarrhoeals & laxative
Anti diarrhoeals & laxative
 
Antibiotics chloramphenicol and macrolides
Antibiotics chloramphenicol and macrolidesAntibiotics chloramphenicol and macrolides
Antibiotics chloramphenicol and macrolides
 
Drug acting on inflammatory bowel disease
Drug acting on inflammatory bowel diseaseDrug acting on inflammatory bowel disease
Drug acting on inflammatory bowel disease
 
Antiamoebic drugs
Antiamoebic drugsAntiamoebic drugs
Antiamoebic drugs
 
Drugs Used in Urinary Tract Infection
Drugs Used in Urinary Tract InfectionDrugs Used in Urinary Tract Infection
Drugs Used in Urinary Tract Infection
 
Serotonin
SerotoninSerotonin
Serotonin
 
peptic ulcer & their new molecular target
peptic ulcer & their new molecular targetpeptic ulcer & their new molecular target
peptic ulcer & their new molecular target
 
Plecanatide
PlecanatidePlecanatide
Plecanatide
 
proton pump inhibitors PPT
proton pump inhibitors PPTproton pump inhibitors PPT
proton pump inhibitors PPT
 
Macrolides
MacrolidesMacrolides
Macrolides
 
Anti emetics
Anti emeticsAnti emetics
Anti emetics
 
Anti ulcer, anti-emetic and prokinetics
Anti ulcer, anti-emetic and prokineticsAnti ulcer, anti-emetic and prokinetics
Anti ulcer, anti-emetic and prokinetics
 
Prokinetics
ProkineticsProkinetics
Prokinetics
 

Similar to Everything You Need to Know About Quinolones

FLUOROQUINOLONES.pptx
FLUOROQUINOLONES.pptxFLUOROQUINOLONES.pptx
FLUOROQUINOLONES.pptxSumeetDumbre
 
Quinolones fluoroquinolones Pharmacology
Quinolones fluoroquinolones PharmacologyQuinolones fluoroquinolones Pharmacology
Quinolones fluoroquinolones PharmacologyKoppala RVS Chaitanya
 
Quinolones and Fluoroquinolone MOA,ADME,Spectrum of activity of Quinolones.
Quinolones and Fluoroquinolone MOA,ADME,Spectrum of activity of Quinolones.Quinolones and Fluoroquinolone MOA,ADME,Spectrum of activity of Quinolones.
Quinolones and Fluoroquinolone MOA,ADME,Spectrum of activity of Quinolones.FahimAnwarRizwi
 
Pharmacology - Quinolones ,Folic Acids Antagonist ,and urinary tract Antiseptics
Pharmacology - Quinolones ,Folic Acids Antagonist ,and urinary tract AntisepticsPharmacology - Quinolones ,Folic Acids Antagonist ,and urinary tract Antiseptics
Pharmacology - Quinolones ,Folic Acids Antagonist ,and urinary tract AntisepticsAreej Abu Hanieh
 
3 (1).ppt, Quinolones, Antibiotcs, Pharmacology
3 (1).ppt, Quinolones, Antibiotcs, Pharmacology3 (1).ppt, Quinolones, Antibiotcs, Pharmacology
3 (1).ppt, Quinolones, Antibiotcs, PharmacologyMaggieAlex1
 
Quinolones and fluroquinolones
Quinolones and fluroquinolonesQuinolones and fluroquinolones
Quinolones and fluroquinoloneszeelmevada
 
Fluoroquinolones
FluoroquinolonesFluoroquinolones
FluoroquinolonesZainab&Sons
 
Fluoroquinolones
FluoroquinolonesFluoroquinolones
FluoroquinolonesZainab&Sons
 
Fluroquinolones 01 01-19
Fluroquinolones 01 01-19Fluroquinolones 01 01-19
Fluroquinolones 01 01-19uma advani
 
6.antibiotics in oral and maxillofacial surgery
6.antibiotics in oral and maxillofacial surgery6.antibiotics in oral and maxillofacial surgery
6.antibiotics in oral and maxillofacial surgeryTejaswini498924
 
DNA Gyrase Inhibitors -quinolones and Fluoroquinolones.pptx
DNA Gyrase Inhibitors -quinolones and Fluoroquinolones.pptxDNA Gyrase Inhibitors -quinolones and Fluoroquinolones.pptx
DNA Gyrase Inhibitors -quinolones and Fluoroquinolones.pptxVijay Salvekar
 
Quinolones & fluoroquinolones
Quinolones & fluoroquinolonesQuinolones & fluoroquinolones
Quinolones & fluoroquinolonesAmeena Kadar
 
DNA Gyrase Inhibitors -Quinolones,Fluoroquinolones
DNA Gyrase Inhibitors -Quinolones,Fluoroquinolones DNA Gyrase Inhibitors -Quinolones,Fluoroquinolones
DNA Gyrase Inhibitors -Quinolones,Fluoroquinolones Vijay Salvekar
 

Similar to Everything You Need to Know About Quinolones (20)

Quinolones.pptx
Quinolones.pptxQuinolones.pptx
Quinolones.pptx
 
Quinolones
QuinolonesQuinolones
Quinolones
 
FLUOROQUINOLONES.pptx
FLUOROQUINOLONES.pptxFLUOROQUINOLONES.pptx
FLUOROQUINOLONES.pptx
 
Quinolones fluoroquinolones Pharmacology
Quinolones fluoroquinolones PharmacologyQuinolones fluoroquinolones Pharmacology
Quinolones fluoroquinolones Pharmacology
 
AMA-_Fluoroqinolones.pdf
AMA-_Fluoroqinolones.pdfAMA-_Fluoroqinolones.pdf
AMA-_Fluoroqinolones.pdf
 
Quinolones and Fluoroquinolone MOA,ADME,Spectrum of activity of Quinolones.
Quinolones and Fluoroquinolone MOA,ADME,Spectrum of activity of Quinolones.Quinolones and Fluoroquinolone MOA,ADME,Spectrum of activity of Quinolones.
Quinolones and Fluoroquinolone MOA,ADME,Spectrum of activity of Quinolones.
 
Pharmacology - Quinolones ,Folic Acids Antagonist ,and urinary tract Antiseptics
Pharmacology - Quinolones ,Folic Acids Antagonist ,and urinary tract AntisepticsPharmacology - Quinolones ,Folic Acids Antagonist ,and urinary tract Antiseptics
Pharmacology - Quinolones ,Folic Acids Antagonist ,and urinary tract Antiseptics
 
3.ppt
3.ppt3.ppt
3.ppt
 
3.ppt
3.ppt3.ppt
3.ppt
 
3 (1).ppt, Quinolones, Antibiotcs, Pharmacology
3 (1).ppt, Quinolones, Antibiotcs, Pharmacology3 (1).ppt, Quinolones, Antibiotcs, Pharmacology
3 (1).ppt, Quinolones, Antibiotcs, Pharmacology
 
Quinolones and fluroquinolones
Quinolones and fluroquinolonesQuinolones and fluroquinolones
Quinolones and fluroquinolones
 
Fluoroquinolones
FluoroquinolonesFluoroquinolones
Fluoroquinolones
 
Fluoroquinolones
FluoroquinolonesFluoroquinolones
Fluoroquinolones
 
Antifungal drugs.pptx
Antifungal drugs.pptxAntifungal drugs.pptx
Antifungal drugs.pptx
 
chinna 21102.pptx
chinna 21102.pptxchinna 21102.pptx
chinna 21102.pptx
 
Fluroquinolones 01 01-19
Fluroquinolones 01 01-19Fluroquinolones 01 01-19
Fluroquinolones 01 01-19
 
6.antibiotics in oral and maxillofacial surgery
6.antibiotics in oral and maxillofacial surgery6.antibiotics in oral and maxillofacial surgery
6.antibiotics in oral and maxillofacial surgery
 
DNA Gyrase Inhibitors -quinolones and Fluoroquinolones.pptx
DNA Gyrase Inhibitors -quinolones and Fluoroquinolones.pptxDNA Gyrase Inhibitors -quinolones and Fluoroquinolones.pptx
DNA Gyrase Inhibitors -quinolones and Fluoroquinolones.pptx
 
Quinolones & fluoroquinolones
Quinolones & fluoroquinolonesQuinolones & fluoroquinolones
Quinolones & fluoroquinolones
 
DNA Gyrase Inhibitors -Quinolones,Fluoroquinolones
DNA Gyrase Inhibitors -Quinolones,Fluoroquinolones DNA Gyrase Inhibitors -Quinolones,Fluoroquinolones
DNA Gyrase Inhibitors -Quinolones,Fluoroquinolones
 

Recently uploaded

zoogeography of pakistan.pptx fauna of Pakistan
zoogeography of pakistan.pptx fauna of Pakistanzoogeography of pakistan.pptx fauna of Pakistan
zoogeography of pakistan.pptx fauna of Pakistanzohaibmir069
 
Neurodevelopmental disorders according to the dsm 5 tr
Neurodevelopmental disorders according to the dsm 5 trNeurodevelopmental disorders according to the dsm 5 tr
Neurodevelopmental disorders according to the dsm 5 trssuser06f238
 
Artificial Intelligence In Microbiology by Dr. Prince C P
Artificial Intelligence In Microbiology by Dr. Prince C PArtificial Intelligence In Microbiology by Dr. Prince C P
Artificial Intelligence In Microbiology by Dr. Prince C PPRINCE C P
 
Disentangling the origin of chemical differences using GHOST
Disentangling the origin of chemical differences using GHOSTDisentangling the origin of chemical differences using GHOST
Disentangling the origin of chemical differences using GHOSTSérgio Sacani
 
Genomic DNA And Complementary DNA Libraries construction.
Genomic DNA And Complementary DNA Libraries construction.Genomic DNA And Complementary DNA Libraries construction.
Genomic DNA And Complementary DNA Libraries construction.k64182334
 
Bentham & Hooker's Classification. along with the merits and demerits of the ...
Bentham & Hooker's Classification. along with the merits and demerits of the ...Bentham & Hooker's Classification. along with the merits and demerits of the ...
Bentham & Hooker's Classification. along with the merits and demerits of the ...Nistarini College, Purulia (W.B) India
 
Dashanga agada a formulation of Agada tantra dealt in 3 Rd year bams agada tanta
Dashanga agada a formulation of Agada tantra dealt in 3 Rd year bams agada tantaDashanga agada a formulation of Agada tantra dealt in 3 Rd year bams agada tanta
Dashanga agada a formulation of Agada tantra dealt in 3 Rd year bams agada tantaPraksha3
 
Analytical Profile of Coleus Forskohlii | Forskolin .pptx
Analytical Profile of Coleus Forskohlii | Forskolin .pptxAnalytical Profile of Coleus Forskohlii | Forskolin .pptx
Analytical Profile of Coleus Forskohlii | Forskolin .pptxSwapnil Therkar
 
Call Girls in Munirka Delhi 💯Call Us 🔝9953322196🔝 💯Escort.
Call Girls in Munirka Delhi 💯Call Us 🔝9953322196🔝 💯Escort.Call Girls in Munirka Delhi 💯Call Us 🔝9953322196🔝 💯Escort.
Call Girls in Munirka Delhi 💯Call Us 🔝9953322196🔝 💯Escort.aasikanpl
 
Hubble Asteroid Hunter III. Physical properties of newly found asteroids
Hubble Asteroid Hunter III. Physical properties of newly found asteroidsHubble Asteroid Hunter III. Physical properties of newly found asteroids
Hubble Asteroid Hunter III. Physical properties of newly found asteroidsSérgio Sacani
 
Grafana in space: Monitoring Japan's SLIM moon lander in real time
Grafana in space: Monitoring Japan's SLIM moon lander in real timeGrafana in space: Monitoring Japan's SLIM moon lander in real time
Grafana in space: Monitoring Japan's SLIM moon lander in real timeSatoshi NAKAHIRA
 
A relative description on Sonoporation.pdf
A relative description on Sonoporation.pdfA relative description on Sonoporation.pdf
A relative description on Sonoporation.pdfnehabiju2046
 
Behavioral Disorder: Schizophrenia & it's Case Study.pdf
Behavioral Disorder: Schizophrenia & it's Case Study.pdfBehavioral Disorder: Schizophrenia & it's Case Study.pdf
Behavioral Disorder: Schizophrenia & it's Case Study.pdfSELF-EXPLANATORY
 
Call Girls in Munirka Delhi 💯Call Us 🔝8264348440🔝
Call Girls in Munirka Delhi 💯Call Us 🔝8264348440🔝Call Girls in Munirka Delhi 💯Call Us 🔝8264348440🔝
Call Girls in Munirka Delhi 💯Call Us 🔝8264348440🔝soniya singh
 
Discovery of an Accretion Streamer and a Slow Wide-angle Outflow around FUOri...
Discovery of an Accretion Streamer and a Slow Wide-angle Outflow around FUOri...Discovery of an Accretion Streamer and a Slow Wide-angle Outflow around FUOri...
Discovery of an Accretion Streamer and a Slow Wide-angle Outflow around FUOri...Sérgio Sacani
 
Recombination DNA Technology (Nucleic Acid Hybridization )
Recombination DNA Technology (Nucleic Acid Hybridization )Recombination DNA Technology (Nucleic Acid Hybridization )
Recombination DNA Technology (Nucleic Acid Hybridization )aarthirajkumar25
 
Animal Communication- Auditory and Visual.pptx
Animal Communication- Auditory and Visual.pptxAnimal Communication- Auditory and Visual.pptx
Animal Communication- Auditory and Visual.pptxUmerFayaz5
 
The Black hole shadow in Modified Gravity
The Black hole shadow in Modified GravityThe Black hole shadow in Modified Gravity
The Black hole shadow in Modified GravitySubhadipsau21168
 

Recently uploaded (20)

zoogeography of pakistan.pptx fauna of Pakistan
zoogeography of pakistan.pptx fauna of Pakistanzoogeography of pakistan.pptx fauna of Pakistan
zoogeography of pakistan.pptx fauna of Pakistan
 
Neurodevelopmental disorders according to the dsm 5 tr
Neurodevelopmental disorders according to the dsm 5 trNeurodevelopmental disorders according to the dsm 5 tr
Neurodevelopmental disorders according to the dsm 5 tr
 
Artificial Intelligence In Microbiology by Dr. Prince C P
Artificial Intelligence In Microbiology by Dr. Prince C PArtificial Intelligence In Microbiology by Dr. Prince C P
Artificial Intelligence In Microbiology by Dr. Prince C P
 
Disentangling the origin of chemical differences using GHOST
Disentangling the origin of chemical differences using GHOSTDisentangling the origin of chemical differences using GHOST
Disentangling the origin of chemical differences using GHOST
 
Genomic DNA And Complementary DNA Libraries construction.
Genomic DNA And Complementary DNA Libraries construction.Genomic DNA And Complementary DNA Libraries construction.
Genomic DNA And Complementary DNA Libraries construction.
 
9953056974 Young Call Girls In Mahavir enclave Indian Quality Escort service
9953056974 Young Call Girls In Mahavir enclave Indian Quality Escort service9953056974 Young Call Girls In Mahavir enclave Indian Quality Escort service
9953056974 Young Call Girls In Mahavir enclave Indian Quality Escort service
 
Bentham & Hooker's Classification. along with the merits and demerits of the ...
Bentham & Hooker's Classification. along with the merits and demerits of the ...Bentham & Hooker's Classification. along with the merits and demerits of the ...
Bentham & Hooker's Classification. along with the merits and demerits of the ...
 
Engler and Prantl system of classification in plant taxonomy
Engler and Prantl system of classification in plant taxonomyEngler and Prantl system of classification in plant taxonomy
Engler and Prantl system of classification in plant taxonomy
 
Dashanga agada a formulation of Agada tantra dealt in 3 Rd year bams agada tanta
Dashanga agada a formulation of Agada tantra dealt in 3 Rd year bams agada tantaDashanga agada a formulation of Agada tantra dealt in 3 Rd year bams agada tanta
Dashanga agada a formulation of Agada tantra dealt in 3 Rd year bams agada tanta
 
Analytical Profile of Coleus Forskohlii | Forskolin .pptx
Analytical Profile of Coleus Forskohlii | Forskolin .pptxAnalytical Profile of Coleus Forskohlii | Forskolin .pptx
Analytical Profile of Coleus Forskohlii | Forskolin .pptx
 
Call Girls in Munirka Delhi 💯Call Us 🔝9953322196🔝 💯Escort.
Call Girls in Munirka Delhi 💯Call Us 🔝9953322196🔝 💯Escort.Call Girls in Munirka Delhi 💯Call Us 🔝9953322196🔝 💯Escort.
Call Girls in Munirka Delhi 💯Call Us 🔝9953322196🔝 💯Escort.
 
Hubble Asteroid Hunter III. Physical properties of newly found asteroids
Hubble Asteroid Hunter III. Physical properties of newly found asteroidsHubble Asteroid Hunter III. Physical properties of newly found asteroids
Hubble Asteroid Hunter III. Physical properties of newly found asteroids
 
Grafana in space: Monitoring Japan's SLIM moon lander in real time
Grafana in space: Monitoring Japan's SLIM moon lander in real timeGrafana in space: Monitoring Japan's SLIM moon lander in real time
Grafana in space: Monitoring Japan's SLIM moon lander in real time
 
A relative description on Sonoporation.pdf
A relative description on Sonoporation.pdfA relative description on Sonoporation.pdf
A relative description on Sonoporation.pdf
 
Behavioral Disorder: Schizophrenia & it's Case Study.pdf
Behavioral Disorder: Schizophrenia & it's Case Study.pdfBehavioral Disorder: Schizophrenia & it's Case Study.pdf
Behavioral Disorder: Schizophrenia & it's Case Study.pdf
 
Call Girls in Munirka Delhi 💯Call Us 🔝8264348440🔝
Call Girls in Munirka Delhi 💯Call Us 🔝8264348440🔝Call Girls in Munirka Delhi 💯Call Us 🔝8264348440🔝
Call Girls in Munirka Delhi 💯Call Us 🔝8264348440🔝
 
Discovery of an Accretion Streamer and a Slow Wide-angle Outflow around FUOri...
Discovery of an Accretion Streamer and a Slow Wide-angle Outflow around FUOri...Discovery of an Accretion Streamer and a Slow Wide-angle Outflow around FUOri...
Discovery of an Accretion Streamer and a Slow Wide-angle Outflow around FUOri...
 
Recombination DNA Technology (Nucleic Acid Hybridization )
Recombination DNA Technology (Nucleic Acid Hybridization )Recombination DNA Technology (Nucleic Acid Hybridization )
Recombination DNA Technology (Nucleic Acid Hybridization )
 
Animal Communication- Auditory and Visual.pptx
Animal Communication- Auditory and Visual.pptxAnimal Communication- Auditory and Visual.pptx
Animal Communication- Auditory and Visual.pptx
 
The Black hole shadow in Modified Gravity
The Black hole shadow in Modified GravityThe Black hole shadow in Modified Gravity
The Black hole shadow in Modified Gravity
 

Everything You Need to Know About Quinolones

  • 2. Quinolones • Synthetic, broad spectrum and bactericidal. • Effective after oral administration for wide variety of infectious diseases, • Play an increasingly important role in treatment of multi-drug resistant bacterial infections. • They are widely used because of their relative safety, availability both orally & parenterally and their favorable pharmacokinetics.
  • 3. • Nalidixic acid was the first quinolone discovered in 1960s and primarily used for urinary tract infection.
  • 4. Fluoroquinolones • Wide variety of application and broad spectrum antibiotic • More potent than quinolones. • Modified quinolones with one or more fluorine atom in their structure.
  • 6. PHARMACOKINETIC • Rapidly and almost completely absorbed after oral administration and are widely distributed in body tissues. • Peak serum levels are obtained within 1- 3 hours of an oral dose of 400mg with peak levels ranging from 1.1 ug/ ml for sparfloxacin to 6.4 ug/ml for levofloxacin . • Food does not impair oral absorption but may delay. • Bioavailability is > 50% for all agents and > 95% for several.
  • 7. • Half life s 3- 5 hours for norfloxacin and ciprofloxacin. • The volume of distribution of quinolones is high with concentration of quinolones n urine, kidney, lung, and prostate tissue, stool, bile and macrophage and neutrophils higher than serum levels. • Concentration in CSF, bone and Prostatic fluid are lower than in serum. • The fluoroquinolones are also metabolized by hepatic conjugation and glucuronidation. Dosage, peak serum levels, percent protein binding, urine concentrations, and degree of metabolism differ to varying degrees among the quinolones.
  • 8. • It is excreted primarily in urine, both by glomerular filtration and tubular secretion. • Urinary and biliary concentrations are 10–50 fold higher than plasma.
  • 9. Mechanism of action • These agents targets DNA gyrase and Topoisomerase IV. • For Gram – ve bacteria DNA gyrase, and for Gram + ve bacteria topoisomerase IV is primary site for their activity. • These drugs binds to A- subunit of DNA gyrases and four subunits of topoisomerase IV enzyme which are responsible for unwinding of supercoiled DNA for process of replication and transcription. • Thus it results in blockade of unwinding and inhibition of replication. • Synthesis of protein inhibited. • inhibition of growth of bacteria and kills bacteria.
  • 10.
  • 11.
  • 12. Antibacterial spectrum • Quinolones have broad spectrum antibacterial activity against various Gram +ve and Gram -ve bacterias including E. coli, Salmonella, Sheigella, P. aeruginosa, Clamydia, mycoplasma, Brucella, Mycobacterium, legionella etc.
  • 13. Antibacterial Resistance • Resistance to the quinolones develops due to mutation to bacterial chromosomal genes of Gyrase A and Topoisomerase IV encoding information to unwind Supercoiled DNA. • No quinolone modifying or inactivating activity has been seen to develop resistance.
  • 14. Therapeutic Uses 1. Urinary tract infections: High cure rates, even in complicated cases or those with indwelling catheters/prostatitis, have been achieved. ChronicPseudomonas infections respond less completely. 2. Gonorrhoea: Initially a single 500 mg dose was nearly 100% curative in non-PPNG as well as PPNG infections, but cure rate has declined in the recent years due to emergence of resistance. 3. Chancroid: 500 mg BD for 3 days is an excellent alternative to ceftriaxone/erythromycin. 4. Bacterial gastroenteritis: Severe cases due toEPEC, Shigella, Salmonella and Campy. jejunirespond quickly. It has also been used to reducestool volume in cholera.
  • 15. 5. Typhoid: Ciprofloxacin is the first choice drug in typhoid fever since chloramphenicol, ampicillin and cotrimoxazole have become unreliable due to development of resistance. A dose of 500–750 mg BD for 10 days is recommended. Patients unable to take the drug orally may be treated with 200 mg. i.v. 12 hourly in the beginning. 6. Bone, soft tissue, gynaecological and wound infections: caused by resistant Staph. and gramnegative bacteria: high cure rates have been obtained but prolonged treatment with high doses is required in osteomyelitis and joint infections.Used along with clindamycin/ metronidazole (to cover anaerobes) it is a good drug for diabetic foot.
  • 16. 7.Respiratory infections: Ciprofloxacin can treat Mycoplasma,, H. influenzae, Branh. catarrhalis and some streptococcal and pneumococcal infections besides gram-negative ones. 8.Tuberculosis It is now frequently used as acomponent of combination chemotherapy against multidrug resistant tuberculosis. Recently, even FQ-resistant TB have arisen. 9.Gram-negative septicaemias: Parenteral ciprofloxacin may be combined with a third generation cephalosporin or an aminoglycoside.
  • 17. • 10. Meningitis: Though penetration in CSF is not very good, ciprofloxacin has been successfully used in gram-negative bacterial meningitis, especially that occurring in immunocompromised patients or those with CSF shunts.
  • 18. Adverse Effects • GI tract- (2–13%) these include nausea, vomiting, diarrhea, and abdominal pain. • CNS effects- (1–8%) such as drowsiness, weakness, headache, dizziness, and in severe cases, convulsions and toxic psychosis, have been reported. • sparfloxacin and lomefloxacinv shows photosensitivity included second-degree burns, discoloration and sometimes permanent discoloration and scarring of the skin due to halogen substitution on the eighth position, as found in
  • 19. • Adverse cardiovascular effects (6–7%; vascular embolism, cardiac insufficiency, hypotension) also occur with sparfloxacin. Sparfloxacin, moxifloxacin, and gatifloxacin can exacerbate QT prolongations. • Fulminant hepatotoxicity associated withtrovafloxacin has resulted in acute liver failure, and the FDA has recommended limiting therapy to life-threateninginfections.
  • 20. • Allergic reactions (e.g., rashes, urticaria, and eosinophilia) have been observed. These drugs have occasionally been associated with cholestatic jaundice, blood dyscrasias, hemolytic anemia, hypoglycemia, and nephrotoxicity. • Recently the use of ciprofloxacin for prophylaxis protection against anthrax infection has been associated with damage to muscle ligaments.
  • 21. Drug Interactions • All quinolones interact with multivalent cations, forming chelation complexes resulting in reduced absorption. • Major offenders are antacids; vitamins containing calcium and iron can also be problematic. All fluoroquinolones interact with warfarin, didanosine, and phenytoin, resulting in decreased absorption or metabolism. • Ciprofloxacin and other second-generation drugs interact with theophylline by decreasing its clearance, which leads to theophylline toxicity.
  • 22. Contraindications • The use of the quinolones in pregnant or breastfeeding women and children whose epiphysial plates have not closed is generally contraindicated. • Their use for treating young cystic fibrosis children infected with Pseudomonas species is an exception; the patient should be monitored carefully for untoward effects.
  • 23. • These drugs contraindicated in arrhythmia because it prolong the heart's QT internal by blocking voltage-gated potassium channels lead to a life-threatening arrhythmia.
  • 24. Nalidixic acid • It is active against gram-negative bacteria, especially E. coli, Proteus, Klebsiella, Enterobacter, Shigella but not Pseudomonas. It acts by inhibiting bacterial DNA gyrase and isbactericidal. • Absorbed orally, highly plasma protein bound and partly metabolized in liver. It is excreted in urine with a plasma t½ ~8 hrs. • Concentration of the free drug in plasma and most tissues attained with the usual doses is non therapeutic • for systemic infections. • Dose: 0.5–1 g TDS or QID
  • 25. Ciprofloxacin • It is the most potent first generation FQ active against a broad range of bacteria, the most susceptible ones are the aerobic gram-negative bacilli, especially the Enterobacteriaceae and Neisseria. • It binds to divalents cations which decreases absorption. • Because of its good penetration into bone, orally administered ciprofloxacin is a useful alternative to parenterally administered antibiotics for the treatment of osteomyelitis caused by susceptible organisms. • Dose- 250, 500, 750 mg tab, 200 mg/100 ml i.v. infusion, 3 mg/ml eye drops.
  • 26. Levofloxacin • It is the levoisomer of ofloxacin having improved activity against Strep. Pneumoniae and some other gram-positive and gramnegative bacteria. • Oral bioavailability of levofloxacin is nearly 100%; oral and i.v. doses are similar. • The primary indication of levofloxacin is community acquired pneumonia and exacerbations of chronic bronchitis in which 87–96% cure rate has been obtained. • High cure rates have been noted in sinusitis, enteric fevers, pyelonephritis and skin/soft tissue infections as well. • Dose- 500 mg tab, 500 mg/100 ml inj.
  • 27. Trovafloxacin • Trovafloxacin is a broad spectrum antibiotic inhibit the uncoiling of supercoiled DNA in various bacteria by blocking the activity of DNA gyrase and topoisomerase IV. • It was shown to be more effective against Gram- positive bacteria than Gram-negative bacteria when compared to previous fluoroquinolones. • Gonorrhea in males and endocervical and rectal gonorrhea in females as well as non gonoccocal urethritis and cervicitis. • Well-absorbed from the gastrointestinal tract after oral administration and does not depend on concomitant food intake. The absolute bioavailability is approximately 88%. • Dose- 300 mg iv and 100 mg tid
  • 28. Repositioning to Anticancer agents • Several FQs just like anyother anticancer drug have been shown to cause cell cycle arrest primarily in S and G2phase of progression. • Several studies reveals the ability of ciprofloxacin to induce S/G2-phase arrest in bladder and prostate cancer cells. Similarly, enoxacin revealed its ability to induce S/G2-phase in prostate cancer cells and G2/M-phase arrest in breast cancer cells. • Later on, few more studies showed similar S/G2-phase arresting effects of other FQs like lomefloxacin, ofloxacin and levofloxacin in epidermoid carcinoma and breast cancer cells respectively. • Ciprofloxacin possesses the maximum efficacy in inducing apoptosis. It shows potent anti-proliferative effect to induce apoptosis in bladder cancer cells and then later on in prostate cancer cells.
  • 29. Clinafloxacin • Methicillin resistant Staphylococcus aureus (MRSA) has developed numerous mechanisms of virulence and strategies to evade the human immune system which are difficult to treat infections in human beings, and becoming important cause of morbidity and mortality. • Acts as novel inhibitors of bacterial efflux pump, FtsZ, DNA gyrase, and topoisomerase IV and have the potential to exert multiple mechanisms of action.
  • 30. Fluoroquinolones in treatment of TB • Fluoroquinolones like moxifloxacin, gatifloxacin and levofloxacin, are the most valuable second- line anti-TB agents according to the current WHO guidelines. • These drugs are currently under clinical trial for pulmonary tuberculosis and tuberculosis meningitis. • The aim of this study is to provide an alternative to resistant drug to prevent failure of treatment and emergence of drug resistance.
  • 31. Delafloxacin in ABSSSI • Delafloxacin is a novel anionic fluoroquinolone (FQ) approved for treatment of acute bacterial skin and skin structure infections (ABSSSIs) caused by a number of Gram-positive and Gram-negative organisms including MRSA and Pseudomonas aeruginosa. • It is more potent than other quinolones against Gram +ve bacteria and Gram –ve bacteria. • It is considered a dual-targeting FQ and displays nearly equivalent affinity for DNA gyrase and topoisomerase IV. • This property likely explains delafloxacin’s broad spectrum of in vitro activity against both GN and GP bacteria
  • 32. Delafloxacin in CABP • Approved for use in adults for the treatment of community-acquired bacterial pneumonia, delafloxacin was shown in a phase III clinical trial to be superior to moxifloxacin in patients with CABP who also have chronic obstructive pulmonary disease (COPD) or asthma as a comorbidity, and in CAP patients who may have severe illness. • Additionally, delafloxacin appeared to be better tolerated compared to commonly used FQs.
  • 33. Levonadifloxacin • It is a novel antibacterial agent belonging to benzoquinolizine subclass of fluoroquinolones which is under clinical development as a parenteral formulation and its prodrug alalevonadifloxacin as an oral option. Both the drugs have been approved recently in India based on phase III trial completed for ABSSSI.
  • 34. Fluoroquinolones in catheter coating • Antimicrobial catheter coatings were prepared by immobilizing fluoroquinolones either with the use of linkers (covalent binding) or by activating the polymer matrix with iodine/bromine (noncovalent binding). • The new antimicrobial coatings, obtained with the participation of fluoroquinolone antibiotics in an uncomplicated way, are able to protect the urinary catheters against bacterial infections during catheterization. • Since the ideal antibacterial material has not yet been found, there is still a need to look for new ways of the prevention of catheter- associated urinary tract infections
  • 35. Sparfloxacin • Ocular diseases affect a growing number of people across the globe. Some pathological ophthalmic conditions, such as glaucoma, diabetic retinopathy, or age-related macular degeneration, cause severe visual impairment that can ultimately lead to blindness. • Nanosuspensions were prepared via a solvent diffusion technique and loaded with sparfloxacin used against bacterial conjunctivitis. • The optimal formulation was the one based on N- carboxymethyl CS nanosuspension in combination with sustainable sparfloxacin release.
  • 36. Antifungal activity • Quinolones and Flouroquinolones displayed potential anti-fungal activity and some of them could significantly increase the susceptibility of antifungals. • Metal complexes of Flouroquinolones with specified antimicrobial activities, are a new entry in the field of bioinorganic. • Zone of inhibition values of fluoroquinolones are compared with parent drug. • Some of them found to exhibit excellent potency against both drug‐susceptible and drug‐resistant fungi where as some found to show lesser or no antifungal behavior as compared to the parent drug.
  • 37. Bioprinting Technology • liver bioengineering has picked up momentum in recent years for the development of both artificial substitutes for supporting repair/regeneration as well as in vitro hepatic models for clinical and diagnostic application. • Trovafloxacin is used to induce liver txicity at tissue level. • Compared to conventional 2D models, trovafloxacin treatment resulted in significant, dose-dependent toxicity at clinically relevant doses (≤4 μM) in the developed 3D models.
  • 38. Sitafloxacin • According to study carried out in Japan : Sitafloxacin based therapy is a potent candidate for third-line Helicobacter pylori eradication treatment. • The 7-day regimen with vonoprazan 20 mg b.i.d., sitafloxacin 100 mg b.i.d., and amoxicillin 750 mg b.i.d. or 500 mg q.i.d. is a good option as the third-line H. pylori eradication treatment
  • 39. Immunomodulatory Effects of Fluoroquinolones • Immune responses are indirectly modulated by FQs through suppressing pro-inflammatory cytokines, such as interleukin 1 (IL-1), IL-6, tumor necrosis factor-alpha (TNF-α), and super-inducing IL-2, which tend to increase both the growth and activity of T and B lymphocytes. In addition, they affect the development of immune responses by influencing of expression of other cytokines and mediators.
  • 40. References • Yadav V, Talwar P, Repositioning of fluoroquinolones from antibiotic to anti-cancer agents: Anunderestimated truth, Biomedicine and pharmacotherapy, 2019, 111, 934- 946. • Xuemei Ge, Zhi Xu, 1,2,4-Triazole hybrids with potential antibacterial activity against methicillin resistant Staphylococcus aureus, Arch Pharm DPhG, 2020, 1- 10. • Dorota Kowalczuk et al, FTIR Characterization of the Development of Antimicrobial Catheter Coatings Loaded with Fluoroquinolones, coating, 2020, 10, 818 • Alexandra Zamboulis et al, Chitosan and its Derivatives for Ocular Delivery Formulations: Recent Advances and Developments, Polymers, 2020, 12, 1519 • Savita Khatria, Manoj Kumara, Pratibha, Rajesh Kumar, A Review of Antifungal Activities of Various Flouroquinolone and Its Metal Complexes, annals of R S C B 2021, 21(5 ), 396- 405 • Tarun Agarwal et al., Recent advances in bioprinting technologies for engineering hepatic tissue, Materials Science & Engineering C, 2021, 123 • Toshihiro Nishizawa et al, Sitafloxacin for Third-Line Helicobacter pylori Eradication: A Systematic Review, J. Clin. Med. 2021, 10, 2722.
  • 41. • Shokrollah Assar et al, A Review of Immunomodulatory Effects of Fluoroquinolones, A Journal of Molecular and Cellular Immunology, 2020 • Pranger AD et al, The Role of fluoroquinolones of in the treatment of tuberculosis 2019, Cross Mark, 2019, 79, 161- 171. • Sharma R, et al, Community Acquired Bacterial Pneumonia- Changing Epidemiology, Resistance Patterns and Newer Antibiotics: Spotlight n Delafloxacin, Clinical drug Investigation, 2020, 40, 947- 960. • Chabner B, Knollman B, Goodman and Gilman’s The Pharmacological Basis of Therapeutics, 12th Edition, 1470 • Tripathi KD, Essentials of Medical Pharmacology, 6th edition, Jaypee Brothers Medical Publishers, 2003, 687. • Craig CR, Stitzel RE, Modern Pharmacology with Clinical Application, 5th Edition, 519.