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Chemotherapy
Outline
• Introduction
• Antibacterial
• Antifungal
• Antiviral
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Chemotherapy
Cont…
Antimicrobial Chemotherapy
• The broad classification of antimicrobial is as
– Antibacterial
– Antifungal
– Antiviral and
– Antiparasitic
• Classification of an antibiotic is based on:
– The class and spectrum of microorganisms it kills
– The biochemical pathway it interferes
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2/9/2023
Antibacterial drugs
• The antibiotics are classified on the basis of the following:
• Chemical structure
– (sulfonamides,
– diamino pyrimidines,
– quinolones,
– β-lactam antibiotics, tetracyclines, nitrobenzene derivatives, macrolides,
lincosamides, glycopeptides, oxazolidinones, polypeptides, nitrofuran derivatives,
nitroimidazoles, azoles, and nicotinic acid derivatives)
• Mechanism of action
– Inhibit cell wall synthesis,
– Disrupt cell membrane,
– Inhibit protein synthesis,
– Inhibit DNA topoisomerase, interfere with DNA function or synthesis, and interfere
with intermediary metabolism)
Cont…
• Spectrum of activity
– narrow spectrum and broad spectrum
• Type of action (bacteriostatic and bactericidal),
• origin (from bacteria, actinomycetes, and fungi)
Cont….
• The choice of an antibacterial is based on considerations of
– pharmacodynamic,
– pharmacokinetic, and
– bacteriological characteristics,
– risk of selecting resistantmutants, and
– cost.
Cell wall synthesis inhibitors
• It is the important cellular structure by which selective toxicity is
achieved.
– With -lactam ring
• Penicillin, Cephalosporin, Monobactams, Carbapenems
– With out -lactam ring
• Vancomycin ,Cyclocerine
2/9/2023 10
Cont…
 Beta-lactam antibiotics
• The inhibit D-alanyl-D-alanine-transpeptidase which essential for
cross linkage of peptidoglycan layer of bacterial cell wall
The bacteria is unable to synthesize a stable cell wall and the it will be lysed
• The group includes
• Penicillin,
• Cephalosporins and
• Carbapenems
2/9/2023 11
Cont…
 Penicillin
• Natural - Penicillin G and V are highly active against
Gram +ve & -ve cocci
But, they are hydrolysed by penicillinase
• The penicillinase-resistant penicillin :
Methicillin, Nafcillin, oxacillin, cloxacillin
Choose for S. aureus and S. epidermidis
• Extended-spectrum penicillin
Ampicillin & amoxicillin
Are effective against gram-ve microorganisms :- H. influenzae, E. coli
and Proteus mirabilis
2/9/2023 12
Cont….
Cephalosporins
• Are β-lactam antibiotics having the same action as penicillins, But
more resistant to certain β-lactamases
• Classified as 1st ,2nd .3rd , 4th & 5th generation, based on their
Bacterial susceptibility patterns and
Resistance to β-lactamases
2/9/2023 13
Cont…
14
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Cont…
Glycopeptides
• Vancomycin and Teicoplanin
• MOA
– Bind to D-alanyl-D-alanine in the growing bacterial cell wall→
inhibits the Transglycosylase,
– Preventing further elongation of peptidoglycan and cross-linking.
• Teicoplanin is two- to fourfold more active than vancomycin
against most Gram-positive cocci
2/9/2023 15
Cont….
• Spectrum of activity
– Aerobic and anaerobic Gram-positive organisms, including
• MSSA and MRSA,
• Streptococci, Enterococci, Corynebacterium spp., Bacillus spp., Listeria
monocytogenes, Clostridium spp.
• Resistance of vancomycin is seen in
– Enterococcus faecalis, E. faecium, and
– Coagulase-ve staphylococci
• Pharmacology
– Parenteral use is limited to IV administration, b/c
• Poorly absorbed after oral administration
• IM administration is extremely painful
– Are eliminated from the body by glomerular filtration
2/9/2023 16
Cont…
• Ophthalmic indications
– Topical, subconjunctival and intravitreal administration For:-
• Infectious corneal ulcers
• Endophthalmitis by G +ve organisms
• Adverse reaction
– Subconjunctival injections may cause conjunctival necrosis and
sloughing.
– Topical administration has also been shown to retard epithelial wound
healing in rabbits
– Ototoxicity, nephrotoxicity
– Rapid infusion causes tingling and flushing of the face, neck, and
thorax ----Redman syndrome
– Hemorrhagic occlusive retinal vasculitis
2/9/2023 17
Cytoplasmic Membrane Inhibitors
• Polymyxin B
• Colistin and
• gramicidin are the antibiotics known to impair the bacterial
cytoplasmic membrane.
Polymyxins
Polymyxins are a group of related cyclic basic polypeptides
originally derived from Bacillus polymyxa
– Interact with the phospholipids in cell mm
– Increases the cell permeability
– Disrupts osmotic integrity
– Leakage of intracellular constituents
– Cell death
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Cont…
• Ophthalmic indications
– Polymyxin B is generally used in combination for Gram-
negative coverage.
• Combinations
– With trimethoprim, bacitracin, or neomycin are available
– With steroid are available for more persistent ocular infections such
as staphylococcal blepharitis.
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Bacterial DNA Synthesis Inhibitors
Fluoroquinolones
• Are bactericidal agents that act by inhibiting DNA replication
• Their targets are enzymes involved in DNA synthesis
– Topoisomerase II (DNA gyrase) and
– Topoisomerase IV
• DNA gyrase exists only in plant and bacterial cells,
– Low toxicity in humans
Cont…
• First generation
– Cinoxacin And Nalidixic Acid
– did not achieve systemic antibacterial levels & were useful
only in lower UTI
• Second generation
– Increased Gram –ve activity, Gram +ve
– Ciprofloxacin is the most potent against P. aeruginosa.
– Ciprofloxacin, Ofloxacin, Norfloxacin, Pefloxacin, Enoxacin,
Lomefloxacin
2/9/2023 22
Cont…
• Third generation
– Levofloxacin, Sparfloxacin, Gatifloxacin
– broad Gram-negative coverage, but less Pseudomonas
coverage
• Fourth generation
– Includes Moxifloxacin, Gemifloxacin, Trovafloxacin
– Have activity against anaerobes and retain activity against
Pseudomonas species
Cont…
• The available topical agents include
– Ciprofloxacin , Ofloxacin , Gatifloxacin (0.3%)
– Levofloxacin (0.5% , 1.5%)
– Moxifloxacin (0.5%) – is with out preservatives
• Have broad spectrum of activity against some gram positives ,
most gram –ve bacteria and anaerobe’s
• Used in treatment of conjunctivitis & corneal ulcers caused by
– S. aureus, S. epidermidis, Streptococcus pneumoniae &
– P. aeruginosa
2/9/2023 24
Cont…
 Pharmacology
• After oral administration, concentrations in serum peak after 1–2h.
• Half-lives of fluoroquinolones range from 3.5h in ciprofloxacin - 20hrs
• Penetrate well into the aqueous humor after topical application.
• Oral or IV administration, widely distributed
• Anatacids ↓ oral bioavailability
2/9/2023 25
Cont…
– 1st & 2nd group quinolones: mainly renal elimination
– 3rd & 4th group quinolones:
• Moxifloxacin: hepatic elimination
• Gemifloxacin: is metabolized to a limited extent by the liver, it is
excreted into the feces & urine
• Gatifloxacin : mainly renal elimination
Cont…
• Ciprofloxacin
– Inhibit 90% of common bacterial corneal pathogens
– Has a lower minimum inhibitory concentration than aminoglycosides and
cefazolin
– Less toxic to the corneal epithelium than aminoglycosides.
• Levofloxacin
– Is an isomer of ofloxacin and
– Has increased activity against Gram +ves,
– But, less potent against P. aeruginosa & certain Enterobacteriaceae.
• Gatifloxacin and moxifloxacin
– Are the newer agents, target both DNA gyrase and topoisomerase IV
– are more active against atypical Mycobacteria, Streptococcus pneumoniae
, S aureus and Staphylococcus epidermidis
2/9/2023 27
Cont…
• Adverse reaction
• Local
– Transient ocular burning or discomfort.
– Ciprofloxacin -> crystalline corneal deposits
– Foreign-body sensation, photophobia, tearing, dry eye, and eye
pain
– Systemic
– Irreversible cartilage erosions and skeletal abnormalities
• Lowest age for usage
– Topical – 2 year
– Systemic – 12 years
2/9/2023 28
Protein Synthesis Inhibitors
• Aminoglycosides,
• Tetracyclines , and
• Macrolide antibiotics as well as
• The individual drugs like
– clindamycin and
– chloramphenicol inhibit the protein synthesis in bacteria.
Cont…
 Aminoglycosides
• Inhibit bacterial protein synthesis by binding irreversibly to the
bacterial 30S ribosomes
• Then become unavailable for translation of mRNA during protein
synthesis, thereby leading to cell death ( bactericidal).
• Aminoglycosides used in ophthalmology are
• Neomycin, Gentamicin, Tobramycin and Amikacin
• Have post antibiotic effect
• Continued suppression of bacterial growth despite the decline of
antimicrobial concentration.
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Cont…
• are active primarily against Aerobic Gram-negative bacilli -
– Enterobacter spp,
– P. aeruginosa, and Acinetobacter spp and
– Staphylococcus aureus
• These agents are only moderately active against Haemophilus
spp. and Neisseria spp.
2/9/2023 31
Cont….
 Pharmacology
• AGs are highly polar
• GI absorption is low with oral aminoglycosides.
• After IV administration they are freely distributed in ECS, but do
not penetrate well into the
– CSF,
– vitreous and
– biliary tract
• Half lives of ∼2–3h
• Excreted by glomerular filtration
– Good renal function is an important factor in their safe use
2/9/2023 32
Cont…
• Have been a mainstay in the treatment of ocular infections.
– However, increasing resistance has limited their use in recent
years.
– Gentamicin and tobramycin - 0.3% topical solutions and
ointments.
• Used for the treatment of severe corneal ulcers, caused by
Pseudomonas spp
2/9/2023 33
Cont…
 Adverse events
• Frequent dosing of fortified aminoglycoside preparations
can result in severe corneal epithelial toxicity.
• Pseudomembranous conjunctivitis is common with
fortified topical gentamicin
• Nephrotoxicity(26%) and ototoxicity(2%)
2/9/2023 34
Cont…
 Tetracyclines
• Inhibit protein synthesis by binding to the 30-S ribosomal so of
polypeptide synthesis
• Are bacteriostatic
• Forms of tetracycline available include
– Chlortetracycline (topical),
– Oxytetracycline,
– Doxycycline and Minocycline
25/10/2010 E.C 35
Cont…
 Pharmacology
• Doxycycline has the best penetration into the eye than others
• Penetration of oxytetracycline and chlortetracycline improved by the
presence of a corneal defect
 Spectrum of activity
• Active against
• Most Gram-positive organisms, Certain Enterobacteriaceae , Chlamydia
spp, Rickettsia spp, Mycobacterium marinum,… and
• Protozoans such as:- Plasmodium spp. and Entamoeba histolytica
• Not usually effective against P. Aeruginosa, bacteroides species, or group B
streptococci.
25/10/2010 E.C 36
Cont…
• Indications
– Prophylaxis for gonococcal ophthalmia neonatorum
– Ocular trachoma
– Against diseases caused by chlamydia, including
• Conjunctivitis, urethritis, cervicitis and pneumonitis
– In treating noninfectious corneal ulceration and acne rosacea
• Adverse events
– Depression of bone growth, Permanent discoloration of the teeth and
– Enamel hypoplasia when given during tooth and skeletal dev’t
• Avoided in children <8 years old and during pregnancy
25/10/2010 E.C 37
Cont…
 Macrolides
• Inhibit bacterial RNA-dependent protein synthesis
• Bind reversibly to the 50S ribosomal subunit blocking peptide
chain elongation
• Includes
– Erythromycin
– Clarithromycin
– Azithromycin
• Spectrum of activity
– Gram-positive cocci & bacilli, Neisseria spp., Mycoplasmas,
Chlamydiae and Propionibacterium acnes
25/10/2010 E.C 38
Cont…
• Erythromycin
• Binds to subunit 50S of bacterial ribosomes and interferes with
proteinsynthesis.
• The drug is bacteriostatic against gram- positive cocci such as
• Streptococcus pyogenes and S pneumoniae,
• gram- positive bacilli such as
• C diphtheriae and
• Listeria monocytogenes, and
• a few gram- negative organisms such as
• N gonorrhea and C trachomatis.
• In sufficient dosing, it may be bactericidal against susceptible organisms.
• Drug re sistance to erythromycin is rising and is as high as 40% among
Streptococcus isolates.
Cont…
• Pharmacology
– Erythromycin is available in
• Topical, Parenteral and Oral preparations
• It is rapidly inactivated by stomach acid
– Metabolism
• Erythromycin and clarithromycin are metabolized by the liver and
excreted in the bile
• Azithromycin is excreted unchanged in the bile.
25/10/2010 E.C 40
Cont….
• Ophthalmic indications
– The topical erythromycin is used for
• Treatment of Chlamydia trachomatis infections
• Prophylaxis of ophthalmia neonatorum
• Conjunctivitis and staphylococcal blepharitis
• As replacement for tetracyclines
• Adverse events
– Erythromycin is one of the safest antibiotics used.
– Side effects are dose-related
• Abdominal cramps, Nausea, Vomiting and diarrhea
25/10/2010 E.C 41
Cont…
• Clarithromycin is more effective against
– Staphylococci, streptococci and M leprae
• Azithromycin is more active against
– H. influenza, N. gonorrhoeae and Chlamydia species
• Both have enhanced activity against
– Mycobacterium avium-intracellulare, Atypical mycobacteria and
– Toxoplasma gondii
– Are more active than erythromycin against chlamydia spp.
25/10/2010 E.C 42
Cont…
 Chloramphenicol
• Inhibits protein synthesis by binding reversibly to the 50S
ribosomal subunit preventing aminoacyl transfer RNA
from binding to the ribosome.
• Active against:- Gram-postve and negatve bacteria,
– Chlamydia, Mycoplasmas and
– Rickettsia
• Effective antibiotic for bacterial conjunctivitis
• Bone marrow toxicity is the major complication of
chloramphenicol use
25/10/2010 E.C 43
Cont…
Sulfonamides
• They are structural analogues of para-aminobenzoic acid (PABA) and
• competitive antagonists of dihydropteroate synthase for the bacterial
synthesis of folic acid.
• Unlike mammals, bacteria cannot use exogenous folic acid but must
synthesize it from PABA.
• Sulfonamides are bacteriostatic only and are more effective when
administered with trimethoprim or
• pyrimethamine each of which is a potent inhibitor of bacterial
dihydrofolate reductase; together, they block successive steps in the
synthesis of folic acid.
Antifungal agents
• The major classes of antifungals used in ophthalmology are
– Polyenes,
– Imidazole
– Pyrimidines
– Echinocandins
• The choice of an antifungal agent depends on
– The primary site of infection,
– The route of administration,
– The organism involved, and
– The sensitivity data available
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Cont…
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Polyenes
• This class of drugs includes amphotericin B (AMB), natamycin,
and nystatin.
• Nystatin is not used routinely to treat ocular infection due to its
low intraocular penetration, toxicity, and resistance to the
drug.
• However, natamycin and amphotericin B are the most
commonly used drugs in cases of fungal keratitis.
Cont…
 Amphotericin B
• A polyene used to control serious fungal infections
• Active against Candida, Aspergillus and Cryptococcus
• Is most commonly used in ophthalmology
• Topically for
Keratitis and scleritis,
2.5-10 mg/mL given every 30-60 min for the first 48-72hr
• Intravitreal (5 μg in 0.1 mL - safe and effective in humans)
Endophthalmitis,
• Systemically (0.5- 1mg/kg/d)
Scleritis, dacryocystitis and cellulitis
48
Cont…
 Natamycin
• The least toxic , least irritating & the most stable of the polyenes
• Available as a 5% suspension
• Has a broad spectrum of sensitivities, especially to fusarium species
• DOC for filamentous fungi
• Has decreased penetration through an intact epithelium
• Topical therapy
• every 30–60 min for the first 48–72 h, and treatment with tapering over
3–6 weeks depending on the activity of the keratitis
• Significant toxicity with Subconj and IV
• It is indicated for fungal
• Conjunctivitis, Blepharitis and Keratitis
49
Cont…
Nystatin
• has been studied experimentally in ophthalmology, and cases
have been reported in which it has been used in external ocular
infections caused by Candida.
• It has been used as a dermatologic ointment, which has a
concentration of 100 000 U/g, and at a frequency of application
every 4–6 h.
• Subconjunctival injections show marked toxicity, and
• experimental intravitreal injection of 0.1 mL of a concentration of
2000 U/mL did not cause a significant reaction and cured an
experimental case of Aspergillus endophthalmitis.
Azoles
• Are the largest class of antimycotics
• Mechanisms
– Inhibit enzyme that convert lanosterol → ergosterol (CYP
P450 14 α- demethylase)
• They have a lower affinity for mammalian P450's
• They are divided into two classes:
– imidazoles which were first to be introduced in the market, and
– followed by triazoles
52
Cont…
 Imidazoles
• The imidazoles have a broad spectrum of antifungal activity.
• At low concentrations, inhibit formation of ergosterol needed by the cell
membranes.
Miconazole, Econazole, And Ketoconazole
• At higher concentrations, can disrupt lysosomes, causing direct damage
to cell membrane.
Clotrimazole And Miconazole
• Most imidazoles inhibit catalase and cytochrome C peroxidase
intracellulary,
– causing accumulation of H2O2--- leading to cell death
53
Cont…
 Ketoconazole
• In ophthalmology,
• Topical and PO ketoconazole has been used clinically and
experimentally for the treatment of keratitis.
• In experimental endophthalmitis, ketoconazole was
effective if started 24 h after injection.
• oral ketoconazole may augment topical natamycin therapy.
54
Cont…
 Miconazole
• It is a broad-spectrum antifungal with activity against
Cryptococcus, Fusarium, Aspergillus, Curvularia, Candida, and
Trichophyton.
• It not only acts on the synthesis of ergosterol but also leads to
• Inhibition of peroxidases, resulting in the accumulation of free
radicals in the fungal cytoplasm which leads to cell death.
• Topical use at a dose of 10 mg/ml or a 1 % solution is effective
especially if associated with epithelial scraping.
• Compared to polyenes, MCZ is less effective but provides better
penetration into ocular tissues
Cont…
Econazole
• Econazole is primarily used in the treatment of superficial mycosis and
not used routinely for the treatment of ocular infections.
• In a clinical trial, 116 eyes with fungal keratitis were randomized to
either econazole 2 % or natamycin 5 %, and
• it was found that econazole is as efficacious as natamycin for the
treatment of fungal keratitis (Prajna et al. 2010).
• However, the drug is not commercially available for
ocular administration which prevents its ophthalmic use.
Triazole
• Fluconazole
• wide spectrum of activity against many pathogens
• The treatment of Candida species
• Able to penetrate intact corneal epithelium, due to its lower MW
• Has efficacy in both topical and oral form against Aspergillus
fumigatus --- In animal studies
• Dose
– Adult = 200 mg/day.
– A topical 1% solution in sterile water can be made
– The 2 mg/L aqueous solution for intravenous use can be applied
topically.
57
Cont…
• Systemic side effects include
– GI upset, headaches, rash, hepatotoxicity, anaphylaxis and
thrombocytopenia.
• Fluconazole
– Can increase cyclosporine's serum concentration and
decrease the metabolism of warfarin
– Rifampin can increase the metabolism of fluconazole
58
Cont…
 Itraconazole
• Is excellent against Aspergillus
• Its spectrum of activity includes
– Candida species,
– Coccidioides and
– Paracoccidioides
– not been very effective against Fusarium.
• Limited use in clinical ophthalmology
• Its oral preparation as an adult dose of 200 mg/day.
• Systemic side effects include:-
– Gastrointestinal upset, hypertriglyceridemia, and hypokalemia
59
Pyrimidines
• Are a group of anti metabolites
Flucytosine (5-FC)
• Is a fluorinated pyrimidine that is soluble in water and alcohol
• It inhibits fungal RNA and DNA synthesis
• Is taken orally at 50-150 mg/kg/ day, divided every 6 hrs.
• Topical 1%-- conjunctivitis, blepharitis, canaliculitis, ant stromal
keratitis.
• Mechanism –enters the cytoplasm by action of cytosine permease
Cytosine deaminase
↓
Flucytocine--------- 5-fluorouracil, and then to 5- fluorodeoxyuridylate.
– This last compound inhibits thymidylate synthase, an important enzyme
in DNA synthesis
60
Newer agents
• Voriconazole
– derived from fluconazole with activity against fluconazole
resistant fungi.
– Can be used orally and IV.
– Its bioavailability is 96%
• Caspofungin
– Inhibits synthesis of B(1,3)-D-glucan, a component of fungal
cell wall.
– Available parenteral
– Invitro activity against various yeasts and molds
61
Antiviral drugs
• Viruses are obligate intracellular parasites that use the
metabolic processes of the invaded host cell.
• Therefore, a major challenge in antiviral therapy has been formulating
antiviral drugs that do not interfere with the normal host-cell
metabolism by causing toxic side effects in the uninfected host cells.
• Theoretically, antiviral drugs may be effective by interacting directly
– with the virus,
– a virus-encoded enzyme or protein,
– a cellular receptor or
– factor required for viral replication or pathogenesis
classification
Cont…
• Twenty antiviral drugs are currently FDA approved for clinical
use, nine with proven efficacy in ocular viral disease:
• vidarabine (Ara-A, Vira A),
• trifluridine(TFT, F3T, Viroptic),
• acyclovir (ACV, Zovirax),
• famciclovir (FCV,Famvir), and valacyclovir (VCV, Valtrex), and
bromovinyldeoxyuridine (BVDU, Brivudine). Ganciclovir
(DHPG*, Cytovene), foscarnet (PFA, Foscavir), and HPMPC
(Cidovir). All but BVDU are FDA approved
CLASSIFICATION OF ANTIVIRAL DRUGS
The viral growth cycle Selective inhibitors
1) Attachment
2) Penetration
-Antiviral antibodies
(gamma globulin)
3) Uncoating -Amantadine, rimantadine
-Interferons
4) Early translation
(early mRNA and protein synthesis)
fomivirsen
5) Transcription
(viral genome replication)
Inhibitors of DNA-polymerase
-Acyclovir -Gancyclovir
-Famcyclovir -Cidofovir
-Vidarabine -Idoxuridine -Trifluridine -
Foscarnet
Inhibitors of RNA-dependent
DNA-polymerase (reverse
transcriptase)
-Zidovudine -Didanosine
-Stavudine -Zalcitabine
-Lamivudine -Foscarnet
6) Late translation
(late mRNA an protein synthesis)
-Ribavirin
-Interferons
7) Posttranslational
modifications
(proteolytic cleavage)
Protease inhibitors
-Saquinavir -Indinavir
-Ritonavir
8) Assembly
(packaging of viral nucleic acids)
-Interferons
-Rifampin
9) Release
(virion is released from cell)
-Antiviral antibodies
-Cytotoxic T lymphocytes
The major sites of antiviral drug action.
Cont…
• Depending on roote of admnistration
• Topical or
• Systemic
Idoxuridine
• It was the first topical antiviral to be used for the treatment of
herpetic epithelial keratitis .
• However, it was later replaced by its thymidine analogue,
trifluridine
• Mechanism of Action IDU
– owes its antiviral activity to the conversion into a triphosphate form, which
mimics thymidine triphosphate and
– becomes incorporated into viral DNA which results in faulty transcription of
viral proteins and inhibition of viral replication.
Trifluridine
• like IDU, is a thymidine analogue which is far more potent and has
less ocular and systemic toxicity.
• Mechanism of Action
– Trifluridine, like IDU, gets converted into a triphosphate
form and gets incorporated into the viral DNA leading to inhibition of
transcriptionand viral protein synthesis.
– Though it also gets incorporated into the host DNA, however, viral DNA
polymerase utilizes trifluridine triphosphate more efficiently than does
host cell DNA polymerase.
– Hence, it has a more selective antiviral activity with lower ocular toxicity
as compared to IDU
Cont…
• Indication
– Trifluridine is active in vitro and in vivo against HSV-1, HSV-2 and
vaccinia and in vitro against CMV and some strains ofadenovirus.
– It is more potent than IDU against HSV.
– It is available as a 1 % solution. Though its penetration is better
than IDU, however, it is not very efficient in iridocyclitis or
stromal keratitis.
– The recommended dosage is one drop every 2 h until healing is
complete.
– This is followed by one drop every 4 h for 7 days to prevent
reactivation of disease
Vidarabine
• Vidarabine was the second agent approved for the topical
treatment of herpetic epithelial keratitis.
• It was also the first antiviral agent approved for systemic use;
however, recently it has been replaced with acyclovir.
Cont…
• Mechanism of Action
• Vidarabine is obtained from fermentation cultures of Streptomyces
antibioticus.
• It is a purine nucleoside analogue that resembles deoxyadenosine.
• It gets converted into its triphosphate form which gets
incorporated into the viral DNA.
• Unlike IDU, trifluridine, or acyclovir, vidarabine does not require viral
thymidine kinase for its phosphorylation.
• Therefore, it might be expected to have high activity against thymidine kinase-
deficient mutants of HSV
Acyclovir
• Acyclovir is a synthetic purine nucleoside analog derived
from guanine.
• It is a highly potent antiviral agent.
• Acyclovir interferes with DNA synthesis, thus inhibiting virus
replication.
• It can be administered both topically and systemically.
• In the topical form it is used as a 3% ointment.
Cont…
• Mechanism of Action
• It is an acyclic analogue of guanosine which is activated by
viral thymidine kinase and becomes a potent inhibitor of viral
DNA polymerase.
• It gets converted into the triphosphate form and is found in
HSV-infected cells in a concentration which is 40–100 times
higher than uninfected cells.
• It has a greater affinity of viral DNA polymerase as compared to
cellular DNA polymerase.
Cont….
• Acyclovir triphosphate inhibits virus growth in 3 ways:
– It can function as a competitive inhibitor of DNA polymerases, with viral
DNA polymerases being significantly more susceptible to acyclovir
triphosphate than are human DNA polymerases.
– It can be a DNA chain terminator.
– It can produce irreversible binding between viral DNA polymerase and
the interrupted chain, causing permanent inactivation.
78
Cont…
Spectrum of activity:
• Antiviral activity against HSV types 1 and 2 (HSV-1 and HSV-2),
VZV, EBV and CMV.
• Topical use of acyclovir ointment is well tolerated.
• Systemic side effects of oral acyclovir include:-
– Nausea, vomiting, and headache.
– Other adverse reactions: diarrhea, dizziness, anorexia, fatigue, edema,
skin rash, leg pain, medication taste, and sore throat.
79
Cont…
• 3% acyclovir may be superior to other antiviral agents with
regards
– To corneal penetration and
– In the treatment of deep herpetic keratitis and uveitis.
• However, acyclovir topical treatment did not significantly
reduce the incidence of stromal keratitis that developed with
herpes simplex epithelial keratitis.
80
Cont…
• For ocular HSV,
– Oral ACV 400 mg 5id is equivalent to topical ACV in treating epithelial
keratitis, with 90% of patients’ ulcers healing in a mean of 5 days.(in
89% of patients on PO and in 97% on Topical)
• PO acyclovir ocular indication
– In patients with HSV keratitis
• as an adjunct to topical antivirals in patients with atopic disease or in
immunosuppressed patients
• Pediatric patients
• Those unable to tolerate topical medication and good RFT
– For preventing recurrence of herpetic disease
– HZO
81
Cont…
• For HZO ACV 800 mg PO 5id for 7–10 days,
• Induces significant resolution of rash, pain, new vesicles and
viral shedding,
• Lower incidence and severity of acute and late dendritiform
keratopathy, scleritis, episcleritis, iritis,
• The incidence but not severity of stromal keratitis
82
Cont…
• Resistance
• There are three mechanisms by which the virus can become
resistant to acyclovir therapy.
• The most common mutation is loss of synthesis of viral
thymidine kinase so that acyclovir is not phosphorylated to its
active form .
• A second type of mutation induces thymidine kinase with
altered substrate specificity that phosphorylates thymidine but
not acyclovir.
• 3rd , a mutation of the viral DNA polymerase gene induces
altered DNA polymerase that is not sensitive to inhibition by
acyclovir triphosphate.
Cont…
Rational Use of Antibiotics
• Antibacterials should be used to only certain definite indications
• Indications for antibacterial therapy
– Definitive therapy
• Narrow spectrum,
• Least toxic and
• Less expensive drug
– Empirical therapy
• To critical cases
• Drugs that cover the most probable infective agent
– Prophylactic therapy
• To susceptible patients
• Narrow spectrum and specific drugs are used
87
Cont…
• Factors that should be considered while prescribing an
antibacterial agent:
• Site & Severity of infection
• Source of infection
• Host factors
• Drug related factors
88
…cont.
• Host factors
– Age
• Infants: CAF is contraindicated
– Not metabolized → ↑concentration blocks electron
transport
• Below the age of 8 years:
– TTCs are CI → discolor the teeth
• Below the age of 12 years:
– Fluoroquinolones are contraindicated
• Elderly: In the elderly
– Drug elimination is slower → dose adjustments
89
Cont…
– Pregnancy:
• TTCs, quinolones, erythromycin and clarithromycin are
CI in all T/Ms
– In lactating mothers
• Tetracyclines, sulfa and quinolones are CI
– Renal failure:
• Tetracyclines , aminoglycosides, cephalosporins &
fluoroquinolones are CI
90
Drug Resistance
• If the maximal level of antibiotic that can be tolerated by the host does
not halt the growth bacteria
• Mechanisms
A. Genetic alterations leading to drug resistance
• DNA undergoes spontaneous mutation
B. Altered expression of proteins
• Modification of target sites
– Alterations in penicillin-binding proteins
• Decreased accumulation
– ↓ed uptake or increased efflux of an antibiotic
• Enzymatic inactivation
91

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Chemotherapy Guide for Antimicrobial Agents

  • 2. Outline • Introduction • Antibacterial • Antifungal • Antiviral 2 2/9/2023
  • 5.
  • 6. Antimicrobial Chemotherapy • The broad classification of antimicrobial is as – Antibacterial – Antifungal – Antiviral and – Antiparasitic • Classification of an antibiotic is based on: – The class and spectrum of microorganisms it kills – The biochemical pathway it interferes 6 2/9/2023
  • 7. Antibacterial drugs • The antibiotics are classified on the basis of the following: • Chemical structure – (sulfonamides, – diamino pyrimidines, – quinolones, – β-lactam antibiotics, tetracyclines, nitrobenzene derivatives, macrolides, lincosamides, glycopeptides, oxazolidinones, polypeptides, nitrofuran derivatives, nitroimidazoles, azoles, and nicotinic acid derivatives) • Mechanism of action – Inhibit cell wall synthesis, – Disrupt cell membrane, – Inhibit protein synthesis, – Inhibit DNA topoisomerase, interfere with DNA function or synthesis, and interfere with intermediary metabolism)
  • 8. Cont… • Spectrum of activity – narrow spectrum and broad spectrum • Type of action (bacteriostatic and bactericidal), • origin (from bacteria, actinomycetes, and fungi)
  • 9. Cont…. • The choice of an antibacterial is based on considerations of – pharmacodynamic, – pharmacokinetic, and – bacteriological characteristics, – risk of selecting resistantmutants, and – cost.
  • 10. Cell wall synthesis inhibitors • It is the important cellular structure by which selective toxicity is achieved. – With -lactam ring • Penicillin, Cephalosporin, Monobactams, Carbapenems – With out -lactam ring • Vancomycin ,Cyclocerine 2/9/2023 10
  • 11. Cont…  Beta-lactam antibiotics • The inhibit D-alanyl-D-alanine-transpeptidase which essential for cross linkage of peptidoglycan layer of bacterial cell wall The bacteria is unable to synthesize a stable cell wall and the it will be lysed • The group includes • Penicillin, • Cephalosporins and • Carbapenems 2/9/2023 11
  • 12. Cont…  Penicillin • Natural - Penicillin G and V are highly active against Gram +ve & -ve cocci But, they are hydrolysed by penicillinase • The penicillinase-resistant penicillin : Methicillin, Nafcillin, oxacillin, cloxacillin Choose for S. aureus and S. epidermidis • Extended-spectrum penicillin Ampicillin & amoxicillin Are effective against gram-ve microorganisms :- H. influenzae, E. coli and Proteus mirabilis 2/9/2023 12
  • 13. Cont…. Cephalosporins • Are β-lactam antibiotics having the same action as penicillins, But more resistant to certain β-lactamases • Classified as 1st ,2nd .3rd , 4th & 5th generation, based on their Bacterial susceptibility patterns and Resistance to β-lactamases 2/9/2023 13
  • 15. Cont… Glycopeptides • Vancomycin and Teicoplanin • MOA – Bind to D-alanyl-D-alanine in the growing bacterial cell wall→ inhibits the Transglycosylase, – Preventing further elongation of peptidoglycan and cross-linking. • Teicoplanin is two- to fourfold more active than vancomycin against most Gram-positive cocci 2/9/2023 15
  • 16. Cont…. • Spectrum of activity – Aerobic and anaerobic Gram-positive organisms, including • MSSA and MRSA, • Streptococci, Enterococci, Corynebacterium spp., Bacillus spp., Listeria monocytogenes, Clostridium spp. • Resistance of vancomycin is seen in – Enterococcus faecalis, E. faecium, and – Coagulase-ve staphylococci • Pharmacology – Parenteral use is limited to IV administration, b/c • Poorly absorbed after oral administration • IM administration is extremely painful – Are eliminated from the body by glomerular filtration 2/9/2023 16
  • 17. Cont… • Ophthalmic indications – Topical, subconjunctival and intravitreal administration For:- • Infectious corneal ulcers • Endophthalmitis by G +ve organisms • Adverse reaction – Subconjunctival injections may cause conjunctival necrosis and sloughing. – Topical administration has also been shown to retard epithelial wound healing in rabbits – Ototoxicity, nephrotoxicity – Rapid infusion causes tingling and flushing of the face, neck, and thorax ----Redman syndrome – Hemorrhagic occlusive retinal vasculitis 2/9/2023 17
  • 18. Cytoplasmic Membrane Inhibitors • Polymyxin B • Colistin and • gramicidin are the antibiotics known to impair the bacterial cytoplasmic membrane.
  • 19. Polymyxins Polymyxins are a group of related cyclic basic polypeptides originally derived from Bacillus polymyxa – Interact with the phospholipids in cell mm – Increases the cell permeability – Disrupts osmotic integrity – Leakage of intracellular constituents – Cell death 19 2/9/2023
  • 20. Cont… • Ophthalmic indications – Polymyxin B is generally used in combination for Gram- negative coverage. • Combinations – With trimethoprim, bacitracin, or neomycin are available – With steroid are available for more persistent ocular infections such as staphylococcal blepharitis. 20 2/9/2023
  • 21. Bacterial DNA Synthesis Inhibitors Fluoroquinolones • Are bactericidal agents that act by inhibiting DNA replication • Their targets are enzymes involved in DNA synthesis – Topoisomerase II (DNA gyrase) and – Topoisomerase IV • DNA gyrase exists only in plant and bacterial cells, – Low toxicity in humans
  • 22. Cont… • First generation – Cinoxacin And Nalidixic Acid – did not achieve systemic antibacterial levels & were useful only in lower UTI • Second generation – Increased Gram –ve activity, Gram +ve – Ciprofloxacin is the most potent against P. aeruginosa. – Ciprofloxacin, Ofloxacin, Norfloxacin, Pefloxacin, Enoxacin, Lomefloxacin 2/9/2023 22
  • 23. Cont… • Third generation – Levofloxacin, Sparfloxacin, Gatifloxacin – broad Gram-negative coverage, but less Pseudomonas coverage • Fourth generation – Includes Moxifloxacin, Gemifloxacin, Trovafloxacin – Have activity against anaerobes and retain activity against Pseudomonas species
  • 24. Cont… • The available topical agents include – Ciprofloxacin , Ofloxacin , Gatifloxacin (0.3%) – Levofloxacin (0.5% , 1.5%) – Moxifloxacin (0.5%) – is with out preservatives • Have broad spectrum of activity against some gram positives , most gram –ve bacteria and anaerobe’s • Used in treatment of conjunctivitis & corneal ulcers caused by – S. aureus, S. epidermidis, Streptococcus pneumoniae & – P. aeruginosa 2/9/2023 24
  • 25. Cont…  Pharmacology • After oral administration, concentrations in serum peak after 1–2h. • Half-lives of fluoroquinolones range from 3.5h in ciprofloxacin - 20hrs • Penetrate well into the aqueous humor after topical application. • Oral or IV administration, widely distributed • Anatacids ↓ oral bioavailability 2/9/2023 25
  • 26. Cont… – 1st & 2nd group quinolones: mainly renal elimination – 3rd & 4th group quinolones: • Moxifloxacin: hepatic elimination • Gemifloxacin: is metabolized to a limited extent by the liver, it is excreted into the feces & urine • Gatifloxacin : mainly renal elimination
  • 27. Cont… • Ciprofloxacin – Inhibit 90% of common bacterial corneal pathogens – Has a lower minimum inhibitory concentration than aminoglycosides and cefazolin – Less toxic to the corneal epithelium than aminoglycosides. • Levofloxacin – Is an isomer of ofloxacin and – Has increased activity against Gram +ves, – But, less potent against P. aeruginosa & certain Enterobacteriaceae. • Gatifloxacin and moxifloxacin – Are the newer agents, target both DNA gyrase and topoisomerase IV – are more active against atypical Mycobacteria, Streptococcus pneumoniae , S aureus and Staphylococcus epidermidis 2/9/2023 27
  • 28. Cont… • Adverse reaction • Local – Transient ocular burning or discomfort. – Ciprofloxacin -> crystalline corneal deposits – Foreign-body sensation, photophobia, tearing, dry eye, and eye pain – Systemic – Irreversible cartilage erosions and skeletal abnormalities • Lowest age for usage – Topical – 2 year – Systemic – 12 years 2/9/2023 28
  • 29. Protein Synthesis Inhibitors • Aminoglycosides, • Tetracyclines , and • Macrolide antibiotics as well as • The individual drugs like – clindamycin and – chloramphenicol inhibit the protein synthesis in bacteria.
  • 30. Cont…  Aminoglycosides • Inhibit bacterial protein synthesis by binding irreversibly to the bacterial 30S ribosomes • Then become unavailable for translation of mRNA during protein synthesis, thereby leading to cell death ( bactericidal). • Aminoglycosides used in ophthalmology are • Neomycin, Gentamicin, Tobramycin and Amikacin • Have post antibiotic effect • Continued suppression of bacterial growth despite the decline of antimicrobial concentration. 2/9/2023 30
  • 31. Cont… • are active primarily against Aerobic Gram-negative bacilli - – Enterobacter spp, – P. aeruginosa, and Acinetobacter spp and – Staphylococcus aureus • These agents are only moderately active against Haemophilus spp. and Neisseria spp. 2/9/2023 31
  • 32. Cont….  Pharmacology • AGs are highly polar • GI absorption is low with oral aminoglycosides. • After IV administration they are freely distributed in ECS, but do not penetrate well into the – CSF, – vitreous and – biliary tract • Half lives of ∼2–3h • Excreted by glomerular filtration – Good renal function is an important factor in their safe use 2/9/2023 32
  • 33. Cont… • Have been a mainstay in the treatment of ocular infections. – However, increasing resistance has limited their use in recent years. – Gentamicin and tobramycin - 0.3% topical solutions and ointments. • Used for the treatment of severe corneal ulcers, caused by Pseudomonas spp 2/9/2023 33
  • 34. Cont…  Adverse events • Frequent dosing of fortified aminoglycoside preparations can result in severe corneal epithelial toxicity. • Pseudomembranous conjunctivitis is common with fortified topical gentamicin • Nephrotoxicity(26%) and ototoxicity(2%) 2/9/2023 34
  • 35. Cont…  Tetracyclines • Inhibit protein synthesis by binding to the 30-S ribosomal so of polypeptide synthesis • Are bacteriostatic • Forms of tetracycline available include – Chlortetracycline (topical), – Oxytetracycline, – Doxycycline and Minocycline 25/10/2010 E.C 35
  • 36. Cont…  Pharmacology • Doxycycline has the best penetration into the eye than others • Penetration of oxytetracycline and chlortetracycline improved by the presence of a corneal defect  Spectrum of activity • Active against • Most Gram-positive organisms, Certain Enterobacteriaceae , Chlamydia spp, Rickettsia spp, Mycobacterium marinum,… and • Protozoans such as:- Plasmodium spp. and Entamoeba histolytica • Not usually effective against P. Aeruginosa, bacteroides species, or group B streptococci. 25/10/2010 E.C 36
  • 37. Cont… • Indications – Prophylaxis for gonococcal ophthalmia neonatorum – Ocular trachoma – Against diseases caused by chlamydia, including • Conjunctivitis, urethritis, cervicitis and pneumonitis – In treating noninfectious corneal ulceration and acne rosacea • Adverse events – Depression of bone growth, Permanent discoloration of the teeth and – Enamel hypoplasia when given during tooth and skeletal dev’t • Avoided in children <8 years old and during pregnancy 25/10/2010 E.C 37
  • 38. Cont…  Macrolides • Inhibit bacterial RNA-dependent protein synthesis • Bind reversibly to the 50S ribosomal subunit blocking peptide chain elongation • Includes – Erythromycin – Clarithromycin – Azithromycin • Spectrum of activity – Gram-positive cocci & bacilli, Neisseria spp., Mycoplasmas, Chlamydiae and Propionibacterium acnes 25/10/2010 E.C 38
  • 39. Cont… • Erythromycin • Binds to subunit 50S of bacterial ribosomes and interferes with proteinsynthesis. • The drug is bacteriostatic against gram- positive cocci such as • Streptococcus pyogenes and S pneumoniae, • gram- positive bacilli such as • C diphtheriae and • Listeria monocytogenes, and • a few gram- negative organisms such as • N gonorrhea and C trachomatis. • In sufficient dosing, it may be bactericidal against susceptible organisms. • Drug re sistance to erythromycin is rising and is as high as 40% among Streptococcus isolates.
  • 40. Cont… • Pharmacology – Erythromycin is available in • Topical, Parenteral and Oral preparations • It is rapidly inactivated by stomach acid – Metabolism • Erythromycin and clarithromycin are metabolized by the liver and excreted in the bile • Azithromycin is excreted unchanged in the bile. 25/10/2010 E.C 40
  • 41. Cont…. • Ophthalmic indications – The topical erythromycin is used for • Treatment of Chlamydia trachomatis infections • Prophylaxis of ophthalmia neonatorum • Conjunctivitis and staphylococcal blepharitis • As replacement for tetracyclines • Adverse events – Erythromycin is one of the safest antibiotics used. – Side effects are dose-related • Abdominal cramps, Nausea, Vomiting and diarrhea 25/10/2010 E.C 41
  • 42. Cont… • Clarithromycin is more effective against – Staphylococci, streptococci and M leprae • Azithromycin is more active against – H. influenza, N. gonorrhoeae and Chlamydia species • Both have enhanced activity against – Mycobacterium avium-intracellulare, Atypical mycobacteria and – Toxoplasma gondii – Are more active than erythromycin against chlamydia spp. 25/10/2010 E.C 42
  • 43. Cont…  Chloramphenicol • Inhibits protein synthesis by binding reversibly to the 50S ribosomal subunit preventing aminoacyl transfer RNA from binding to the ribosome. • Active against:- Gram-postve and negatve bacteria, – Chlamydia, Mycoplasmas and – Rickettsia • Effective antibiotic for bacterial conjunctivitis • Bone marrow toxicity is the major complication of chloramphenicol use 25/10/2010 E.C 43
  • 44. Cont… Sulfonamides • They are structural analogues of para-aminobenzoic acid (PABA) and • competitive antagonists of dihydropteroate synthase for the bacterial synthesis of folic acid. • Unlike mammals, bacteria cannot use exogenous folic acid but must synthesize it from PABA. • Sulfonamides are bacteriostatic only and are more effective when administered with trimethoprim or • pyrimethamine each of which is a potent inhibitor of bacterial dihydrofolate reductase; together, they block successive steps in the synthesis of folic acid.
  • 45. Antifungal agents • The major classes of antifungals used in ophthalmology are – Polyenes, – Imidazole – Pyrimidines – Echinocandins • The choice of an antifungal agent depends on – The primary site of infection, – The route of administration, – The organism involved, and – The sensitivity data available 45 2/9/2023
  • 47. Polyenes • This class of drugs includes amphotericin B (AMB), natamycin, and nystatin. • Nystatin is not used routinely to treat ocular infection due to its low intraocular penetration, toxicity, and resistance to the drug. • However, natamycin and amphotericin B are the most commonly used drugs in cases of fungal keratitis.
  • 48. Cont…  Amphotericin B • A polyene used to control serious fungal infections • Active against Candida, Aspergillus and Cryptococcus • Is most commonly used in ophthalmology • Topically for Keratitis and scleritis, 2.5-10 mg/mL given every 30-60 min for the first 48-72hr • Intravitreal (5 μg in 0.1 mL - safe and effective in humans) Endophthalmitis, • Systemically (0.5- 1mg/kg/d) Scleritis, dacryocystitis and cellulitis 48
  • 49. Cont…  Natamycin • The least toxic , least irritating & the most stable of the polyenes • Available as a 5% suspension • Has a broad spectrum of sensitivities, especially to fusarium species • DOC for filamentous fungi • Has decreased penetration through an intact epithelium • Topical therapy • every 30–60 min for the first 48–72 h, and treatment with tapering over 3–6 weeks depending on the activity of the keratitis • Significant toxicity with Subconj and IV • It is indicated for fungal • Conjunctivitis, Blepharitis and Keratitis 49
  • 50. Cont… Nystatin • has been studied experimentally in ophthalmology, and cases have been reported in which it has been used in external ocular infections caused by Candida. • It has been used as a dermatologic ointment, which has a concentration of 100 000 U/g, and at a frequency of application every 4–6 h. • Subconjunctival injections show marked toxicity, and • experimental intravitreal injection of 0.1 mL of a concentration of 2000 U/mL did not cause a significant reaction and cured an experimental case of Aspergillus endophthalmitis.
  • 51.
  • 52. Azoles • Are the largest class of antimycotics • Mechanisms – Inhibit enzyme that convert lanosterol → ergosterol (CYP P450 14 α- demethylase) • They have a lower affinity for mammalian P450's • They are divided into two classes: – imidazoles which were first to be introduced in the market, and – followed by triazoles 52
  • 53. Cont…  Imidazoles • The imidazoles have a broad spectrum of antifungal activity. • At low concentrations, inhibit formation of ergosterol needed by the cell membranes. Miconazole, Econazole, And Ketoconazole • At higher concentrations, can disrupt lysosomes, causing direct damage to cell membrane. Clotrimazole And Miconazole • Most imidazoles inhibit catalase and cytochrome C peroxidase intracellulary, – causing accumulation of H2O2--- leading to cell death 53
  • 54. Cont…  Ketoconazole • In ophthalmology, • Topical and PO ketoconazole has been used clinically and experimentally for the treatment of keratitis. • In experimental endophthalmitis, ketoconazole was effective if started 24 h after injection. • oral ketoconazole may augment topical natamycin therapy. 54
  • 55. Cont…  Miconazole • It is a broad-spectrum antifungal with activity against Cryptococcus, Fusarium, Aspergillus, Curvularia, Candida, and Trichophyton. • It not only acts on the synthesis of ergosterol but also leads to • Inhibition of peroxidases, resulting in the accumulation of free radicals in the fungal cytoplasm which leads to cell death. • Topical use at a dose of 10 mg/ml or a 1 % solution is effective especially if associated with epithelial scraping. • Compared to polyenes, MCZ is less effective but provides better penetration into ocular tissues
  • 56. Cont… Econazole • Econazole is primarily used in the treatment of superficial mycosis and not used routinely for the treatment of ocular infections. • In a clinical trial, 116 eyes with fungal keratitis were randomized to either econazole 2 % or natamycin 5 %, and • it was found that econazole is as efficacious as natamycin for the treatment of fungal keratitis (Prajna et al. 2010). • However, the drug is not commercially available for ocular administration which prevents its ophthalmic use.
  • 57. Triazole • Fluconazole • wide spectrum of activity against many pathogens • The treatment of Candida species • Able to penetrate intact corneal epithelium, due to its lower MW • Has efficacy in both topical and oral form against Aspergillus fumigatus --- In animal studies • Dose – Adult = 200 mg/day. – A topical 1% solution in sterile water can be made – The 2 mg/L aqueous solution for intravenous use can be applied topically. 57
  • 58. Cont… • Systemic side effects include – GI upset, headaches, rash, hepatotoxicity, anaphylaxis and thrombocytopenia. • Fluconazole – Can increase cyclosporine's serum concentration and decrease the metabolism of warfarin – Rifampin can increase the metabolism of fluconazole 58
  • 59. Cont…  Itraconazole • Is excellent against Aspergillus • Its spectrum of activity includes – Candida species, – Coccidioides and – Paracoccidioides – not been very effective against Fusarium. • Limited use in clinical ophthalmology • Its oral preparation as an adult dose of 200 mg/day. • Systemic side effects include:- – Gastrointestinal upset, hypertriglyceridemia, and hypokalemia 59
  • 60. Pyrimidines • Are a group of anti metabolites Flucytosine (5-FC) • Is a fluorinated pyrimidine that is soluble in water and alcohol • It inhibits fungal RNA and DNA synthesis • Is taken orally at 50-150 mg/kg/ day, divided every 6 hrs. • Topical 1%-- conjunctivitis, blepharitis, canaliculitis, ant stromal keratitis. • Mechanism –enters the cytoplasm by action of cytosine permease Cytosine deaminase ↓ Flucytocine--------- 5-fluorouracil, and then to 5- fluorodeoxyuridylate. – This last compound inhibits thymidylate synthase, an important enzyme in DNA synthesis 60
  • 61. Newer agents • Voriconazole – derived from fluconazole with activity against fluconazole resistant fungi. – Can be used orally and IV. – Its bioavailability is 96% • Caspofungin – Inhibits synthesis of B(1,3)-D-glucan, a component of fungal cell wall. – Available parenteral – Invitro activity against various yeasts and molds 61
  • 62.
  • 63.
  • 64. Antiviral drugs • Viruses are obligate intracellular parasites that use the metabolic processes of the invaded host cell. • Therefore, a major challenge in antiviral therapy has been formulating antiviral drugs that do not interfere with the normal host-cell metabolism by causing toxic side effects in the uninfected host cells. • Theoretically, antiviral drugs may be effective by interacting directly – with the virus, – a virus-encoded enzyme or protein, – a cellular receptor or – factor required for viral replication or pathogenesis
  • 66. Cont… • Twenty antiviral drugs are currently FDA approved for clinical use, nine with proven efficacy in ocular viral disease: • vidarabine (Ara-A, Vira A), • trifluridine(TFT, F3T, Viroptic), • acyclovir (ACV, Zovirax), • famciclovir (FCV,Famvir), and valacyclovir (VCV, Valtrex), and bromovinyldeoxyuridine (BVDU, Brivudine). Ganciclovir (DHPG*, Cytovene), foscarnet (PFA, Foscavir), and HPMPC (Cidovir). All but BVDU are FDA approved
  • 67. CLASSIFICATION OF ANTIVIRAL DRUGS The viral growth cycle Selective inhibitors 1) Attachment 2) Penetration -Antiviral antibodies (gamma globulin) 3) Uncoating -Amantadine, rimantadine -Interferons 4) Early translation (early mRNA and protein synthesis) fomivirsen 5) Transcription (viral genome replication) Inhibitors of DNA-polymerase -Acyclovir -Gancyclovir -Famcyclovir -Cidofovir -Vidarabine -Idoxuridine -Trifluridine - Foscarnet Inhibitors of RNA-dependent DNA-polymerase (reverse transcriptase) -Zidovudine -Didanosine -Stavudine -Zalcitabine -Lamivudine -Foscarnet
  • 68. 6) Late translation (late mRNA an protein synthesis) -Ribavirin -Interferons 7) Posttranslational modifications (proteolytic cleavage) Protease inhibitors -Saquinavir -Indinavir -Ritonavir 8) Assembly (packaging of viral nucleic acids) -Interferons -Rifampin 9) Release (virion is released from cell) -Antiviral antibodies -Cytotoxic T lymphocytes
  • 69. The major sites of antiviral drug action.
  • 70. Cont… • Depending on roote of admnistration • Topical or • Systemic
  • 71. Idoxuridine • It was the first topical antiviral to be used for the treatment of herpetic epithelial keratitis . • However, it was later replaced by its thymidine analogue, trifluridine • Mechanism of Action IDU – owes its antiviral activity to the conversion into a triphosphate form, which mimics thymidine triphosphate and – becomes incorporated into viral DNA which results in faulty transcription of viral proteins and inhibition of viral replication.
  • 72. Trifluridine • like IDU, is a thymidine analogue which is far more potent and has less ocular and systemic toxicity. • Mechanism of Action – Trifluridine, like IDU, gets converted into a triphosphate form and gets incorporated into the viral DNA leading to inhibition of transcriptionand viral protein synthesis. – Though it also gets incorporated into the host DNA, however, viral DNA polymerase utilizes trifluridine triphosphate more efficiently than does host cell DNA polymerase. – Hence, it has a more selective antiviral activity with lower ocular toxicity as compared to IDU
  • 73. Cont… • Indication – Trifluridine is active in vitro and in vivo against HSV-1, HSV-2 and vaccinia and in vitro against CMV and some strains ofadenovirus. – It is more potent than IDU against HSV. – It is available as a 1 % solution. Though its penetration is better than IDU, however, it is not very efficient in iridocyclitis or stromal keratitis. – The recommended dosage is one drop every 2 h until healing is complete. – This is followed by one drop every 4 h for 7 days to prevent reactivation of disease
  • 74. Vidarabine • Vidarabine was the second agent approved for the topical treatment of herpetic epithelial keratitis. • It was also the first antiviral agent approved for systemic use; however, recently it has been replaced with acyclovir.
  • 75. Cont… • Mechanism of Action • Vidarabine is obtained from fermentation cultures of Streptomyces antibioticus. • It is a purine nucleoside analogue that resembles deoxyadenosine. • It gets converted into its triphosphate form which gets incorporated into the viral DNA. • Unlike IDU, trifluridine, or acyclovir, vidarabine does not require viral thymidine kinase for its phosphorylation. • Therefore, it might be expected to have high activity against thymidine kinase- deficient mutants of HSV
  • 76. Acyclovir • Acyclovir is a synthetic purine nucleoside analog derived from guanine. • It is a highly potent antiviral agent. • Acyclovir interferes with DNA synthesis, thus inhibiting virus replication. • It can be administered both topically and systemically. • In the topical form it is used as a 3% ointment.
  • 77. Cont… • Mechanism of Action • It is an acyclic analogue of guanosine which is activated by viral thymidine kinase and becomes a potent inhibitor of viral DNA polymerase. • It gets converted into the triphosphate form and is found in HSV-infected cells in a concentration which is 40–100 times higher than uninfected cells. • It has a greater affinity of viral DNA polymerase as compared to cellular DNA polymerase.
  • 78. Cont…. • Acyclovir triphosphate inhibits virus growth in 3 ways: – It can function as a competitive inhibitor of DNA polymerases, with viral DNA polymerases being significantly more susceptible to acyclovir triphosphate than are human DNA polymerases. – It can be a DNA chain terminator. – It can produce irreversible binding between viral DNA polymerase and the interrupted chain, causing permanent inactivation. 78
  • 79. Cont… Spectrum of activity: • Antiviral activity against HSV types 1 and 2 (HSV-1 and HSV-2), VZV, EBV and CMV. • Topical use of acyclovir ointment is well tolerated. • Systemic side effects of oral acyclovir include:- – Nausea, vomiting, and headache. – Other adverse reactions: diarrhea, dizziness, anorexia, fatigue, edema, skin rash, leg pain, medication taste, and sore throat. 79
  • 80. Cont… • 3% acyclovir may be superior to other antiviral agents with regards – To corneal penetration and – In the treatment of deep herpetic keratitis and uveitis. • However, acyclovir topical treatment did not significantly reduce the incidence of stromal keratitis that developed with herpes simplex epithelial keratitis. 80
  • 81. Cont… • For ocular HSV, – Oral ACV 400 mg 5id is equivalent to topical ACV in treating epithelial keratitis, with 90% of patients’ ulcers healing in a mean of 5 days.(in 89% of patients on PO and in 97% on Topical) • PO acyclovir ocular indication – In patients with HSV keratitis • as an adjunct to topical antivirals in patients with atopic disease or in immunosuppressed patients • Pediatric patients • Those unable to tolerate topical medication and good RFT – For preventing recurrence of herpetic disease – HZO 81
  • 82. Cont… • For HZO ACV 800 mg PO 5id for 7–10 days, • Induces significant resolution of rash, pain, new vesicles and viral shedding, • Lower incidence and severity of acute and late dendritiform keratopathy, scleritis, episcleritis, iritis, • The incidence but not severity of stromal keratitis 82
  • 83. Cont… • Resistance • There are three mechanisms by which the virus can become resistant to acyclovir therapy. • The most common mutation is loss of synthesis of viral thymidine kinase so that acyclovir is not phosphorylated to its active form . • A second type of mutation induces thymidine kinase with altered substrate specificity that phosphorylates thymidine but not acyclovir. • 3rd , a mutation of the viral DNA polymerase gene induces altered DNA polymerase that is not sensitive to inhibition by acyclovir triphosphate.
  • 85.
  • 86.
  • 87. Rational Use of Antibiotics • Antibacterials should be used to only certain definite indications • Indications for antibacterial therapy – Definitive therapy • Narrow spectrum, • Least toxic and • Less expensive drug – Empirical therapy • To critical cases • Drugs that cover the most probable infective agent – Prophylactic therapy • To susceptible patients • Narrow spectrum and specific drugs are used 87
  • 88. Cont… • Factors that should be considered while prescribing an antibacterial agent: • Site & Severity of infection • Source of infection • Host factors • Drug related factors 88
  • 89. …cont. • Host factors – Age • Infants: CAF is contraindicated – Not metabolized → ↑concentration blocks electron transport • Below the age of 8 years: – TTCs are CI → discolor the teeth • Below the age of 12 years: – Fluoroquinolones are contraindicated • Elderly: In the elderly – Drug elimination is slower → dose adjustments 89
  • 90. Cont… – Pregnancy: • TTCs, quinolones, erythromycin and clarithromycin are CI in all T/Ms – In lactating mothers • Tetracyclines, sulfa and quinolones are CI – Renal failure: • Tetracyclines , aminoglycosides, cephalosporins & fluoroquinolones are CI 90
  • 91. Drug Resistance • If the maximal level of antibiotic that can be tolerated by the host does not halt the growth bacteria • Mechanisms A. Genetic alterations leading to drug resistance • DNA undergoes spontaneous mutation B. Altered expression of proteins • Modification of target sites – Alterations in penicillin-binding proteins • Decreased accumulation – ↓ed uptake or increased efflux of an antibiotic • Enzymatic inactivation 91