Last zatchot/ Bacteria - viruses - fungai - Plasmudium Flashcards
Explain Classification of Antibiotics drugs ( Cell water inhibitors) , penicillin’s mechanism of action , resistance of Penicillin, pharmacokinetics
—Classification of Cell wall inhibitors
1-Penicillin
2-Cephalosporin
3-Monobactams
4-Carbapenems
5-Glycopeotides
— Penicillin mechanism :
The mechanism is for all penicillins groups is the same , Penicillin bind to (PBP - Penicillin binding protein ) on the bacterial cell wall and inhibits the transpeptidse enzyme which is inhibite the transpeptades reaction , which is synthesis the walls of the cell , then it’s activates the autolytic enzyme called autolysin leading to cell rapture which is result of of cell wall inhibition and autolysis
-NB! The penicillin mechanism requires proliferation microorganisms, have no effect of bacteria that not dividing
—Penicillin resistant:
Enzymatic hydrolysis of the beta-lactam ring results in loss
of antibacterial activity. The formation of beta-lactamases
(penicillinases) by most staphylococci and many Gram-negative
organisms is a major mechanism of bacterial resistance. Inhibitors of these bacterial enzymes (eg, clavulanic acid, sulbactam, tazobactam) are often used in combination with penicillins to prevent their inactivation. Structural change in target PBPs is another mechanism of resistance and is responsible for methicillin resistance in staphylococci and for resistance to penicillin G in pneumococci (eg, PRSP, penicillin resistant Streptococcus pneumoniae)
and enterococci. In some Gram-negative rods (eg, Pseudomonas
aeruginosa), changes in the porin structures in the outer cell wall membrane may contribute to resistance by impeding access of penicillins to PBPs
1-MRSA ( methilin resistant staphylococcus aureus )
2-Some E-Coli
3-Psudomons
4-some streptococci
—- Penicillin Pharmacokinetics:
-Some penicillin should be Givin :
IV , IM , orally
-distribution: penicillin normally is non-ionised but once it reach the blood PH 7,47 become ionised and can’t pass BBB except in case which is meningitis due to tight junction gets dilated duo to inflammation so the Penicillin can reach the BBB
- penicillin can cross placenta but its not tetroginc bcs the fetal tissue has no Transpeptidase enzyme / PBP
-Excretion : mostly renal
classification of Penicillin drugs
-Natural :
1- Benzylpenicillin ( Penicillin G) short acting -Parenteral
2-Phenoxymethylpenicillin
(penicillin V) Orally - Short acting
3-Benzathine BenzylPencillin ( long acting per 7d - IM)
-Semi - Synthetic :
1-Anti Staphylococci Penicillin: Oxacilln
2-Extended Spectrum Penicillin:
Ampicillin - Amoxicillin
3-Antipsudomonal Pencillin :
Piperacillin , Ticarcillin
Explain BenzylPenicillin , Spectrum , list of bacteria , disadvantage
-Drug : Benzylpenicillin amp 1mlion ED
-Its the original Penicillin
-Spectrum : Narrow spectrum duo to targeting few Gram + bacteria only such as :
1-Streptococci
2-P.Coccai
3-Some staphylococci which is not producing B-Lactamse
4-Gono coccai : Gonnoria : Gram-
5-Treponin pellidum ( Sophylis) gram-
-disadvantage:
1-Cant be orally bcs HCL
2-Half life 2-4h ( shorty acting )
3- B-lactamse enzyme sensitivity
4-Narrow spectrum
Explain Phenoxymethylpenicillin ( Penicillin V) , Benzathine Benzylpenicillin ,Anti-Staphylococcal, Drug , spectrum, resistance,
-Drug : Phenoxymethylpenicillin Tab0.25 Penicillin V
-Its the same as Penicillin G , But its acid stable , Also short acting , and narrow spectrum
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-Drug : Benzathine Benzylpenicillin
-Its the same as penicillin G but with modification which makes it last longer 7-14 days
- its most used in prophylaxis and treatment of syphalis during pregnancy
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-,Anti-Staphylococcal,
-Drug : Oxacillin Tab/Amp 0,25/0,5
-they are effective against B-Lacatmes producing Staphylococci , But they have no effect or low activity against
other Gram- and Gram+ bacteria: Narrow spectrum .
-They most used against MRSA only
Explain Extended Spectrum penicillin , antibiotic drugs , B-Lcatamse inhibitors drugs , Spectrum, List of bacteria , ROA , resistance, Combination with B-Lcatamse inhibitors, , mechanism of Gram- , difference between Ampicillin and Amoxicillin
-Antibiotic drugs : , B-Lctms inhbt
1-Ampicillin + Sulbactam Amp 0,5/0,25
2-Amoxicillin + Clavulanic Acid Tab 0,25/0,6
-Spectrum : they are narrow/moderate spectrum duo to coverage of G+,G- Such as :
1-Slamonila
2-H.influenza
3-Protus
4-Shigella
-ROA : they are acid stable so they can be orally
-resistant: they are sensitive to B-Lactamse , and thats why we give them in combination with B-Lactamse inhibitors
-Mechanism of acting on Gram- :
The ampicillin/Amoxicillin have NH2 group : Amino acid,so it can pass the pores of the outer membrane as nutrients, and destroy the Cell wall and activate Autolysin
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-Ampicillin:
1-oral absorption: +
2-distribution :+
3-Diarrhoea : +++ bcs its not absorbed 100% so it kills the bacteria in the GI
4-Spectrum : shigella , H.influenza
———
Amoxicillin :
1-oral absorption: ++
2-distribution :++ more in lung
3-Diarrhoea :+
4-Spectrum : Salmonila/typhoid fever ,
H,Pylori , Streptococcus pneumonia
Explain Anti-Pesudmonal penicillin, Drugs , spectrum, resistance
-Drugs :
1-piperacillin , Ticarcillin Amp
-Spectrum: they are targeting pseudomonal (Mainly) , Also G+ and G- also anaerobic bacteria, so they are broad spectrum
-resistant: they are B-Lactamase sensitive thats why we should combine it with Sulbactam ( b lactamse inhibitor )
What are the uses of Penicillin
1-Streptococcal infection: wound spesis , tonsillitis, sub endocrdaitis
2-P.Coccoi : pneumonia
3-Syphalis , Gonnoria
4-Minigialcoccai : meningitis
5-Typhoid fever
6-Pesudomons
7-Actinomycosis ,Anthrax , H.Influenza
Explain side effect of penicillin and drug interactions
—Side effect :
1-Allergic reaction : it occurs with all types of penicillin, and its not duo to penicillin it self but to degradation products common to all penicillin it more commonly in parental
2-Diarrhea: disruption of the balance of intestinal
microorganisms. It occurs to a greater extent with those
agents that are incompletely absorbed and have an
extended antibacterial spectrum. Pseudomembranous
colitis from Clostridium difficile may occur with penicillin use
3-Nephritis
4–Neurotoxicity: The penicillins can provoke seizures if injectedintrathecally or if very high blood levels. Epileptic patients are particularly at risk due to the ability of penicillins to cause GABAergic inhibition
– Drug intractions :
1-bactriostatics : bcs the penicillin need prolofration to act
2-Anti-pesudomonal with aminoglycosides : bcs they are diffreant in charge puting them in one syrngist they will make complex and antagonise each other
Explain the cephalosporin, structure,generation,,Pharmacokinetics,
-Cephalosporin Also a B-lactamse ring have similar mechanism of action As penicillin
-Each newer generation increasingly resistant to B-Lactamse .
-Pharmacoinatic :
-Distribution:They are widely distributed,But 3rd ,4th,5th generation can Penetrate CSF
-Ceftriaxone 3rd gen , are mainly excreted by bile
Explain 1st-5th generation of Cephalosporin, Spectrum,Resistance,BBB,allergy
1St Gen
-Drugs :
1-Cefazolin amp 0.5 2-Cefalexine tab
-Spectrum: narrow spectrum, duo to covering G+ same as Penicillin G with some G- ( E coli klebsiella )
-resistant: Sensitive to B-Lactamse
-BBB : Dont pass
-Allergy : Cross allergy with Penicillin
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2nd Gen
-Drugs : Cefuroxime Tab/Amp
-Spectrum : Covering G+ and some G- such as ( H.Influenza,Neaseria , Proteus ) but not Pesudomons , Narrow spectrum
-Resistant : Reletavly resistant to B-Lactamse
-BBB: only Cefuroxime Can pss
-Allergy : Cross allergy with penicillin
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3rd Gen
-Drugs :
1-Oral :
-Cefixime
-Ceftibutene
2-Parenteral :
-Cefotaxime
-Ceftriaxone
-Ceftazidime
—Spectrum: mainly Gram- and also a few of Gram+ ,Also active aginst psudomonas , And anaerobic , Moderate spectrum
-Resistant: Resistant to B-Lactramse
-BBB : Pass BBB
-Allergy: No cross allergy with Penicillin
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4th Gen
-Drugs : Cefepime Amp 0.5
—Spectrum: Coverse G+,G- , Pusdomonas , Also anaerobic , Broad spectrum
-Resistant: highly resistant to B-Lactamse
-BBB : Pass BBB
-Allergy: No cross allergy with Penicillin
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5th Gen
-Drugs : Ceftaroline Amp 0.5
—Spectrum: Coverse G+,G- , Pusdomonas , Also anaerobic ,MRSA, Broad spectrum
-Resistant: highly resistant to B-Lactamse
-BBB : Pass BBB
-Allergy: No cross allergy with Penicillin
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mechansim of resistance for cephalosporins
Structural differences from penicillins render cephalosporins
less susceptible to penicillinases produced by staphylococci, but many bacteria are resistant through the production of other betalactamases that can inactivate cephalosporins. Resistance can also result from decreases in membrane permeability to cephalosporins and from changes in PBPs. Methicillin-resistant staphylococci are also resistant to cephalosporins.
Uses of Cephalosporin + Side effect
-Most urgent :
1-Meningitis -ve
2-Osteomyelitis
3-Skin infection
4-Typhoid fever
5- UTI : E-Coli -Ve
6-Rsp infection
7-Gannoria
8-ENT
9-intestinal infection
10-Topical
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-Side effect :
1-Nephrotoxince : Most of them is 1gen
-VIP-2-Disulferam like action : normally alcohol > Acetyldhayed > Co2 and H2o, by the help of Aldahyed dehydrogenase , so these drugs inhibit aldehyide dehydrogenase which results of bad mood and nause and vomiting is also ( Drug interaction)
-VIP-3-Prothrombin : 3rd generation inhibt the enzyme Vit k exopidese lead to hypoprothrombinemia
Explain Monobactams , Drug , structure , Spectrum, Allergy
-Drug : Aztreonam amp 0.5
-Structure : B-lactam ring similar to Penicillin
-Spectrum: Narrow spectrum, Only Gram-
-resistant: highly resistant
-Allergy: no allergy at all
Explain Carbapenems,Drugs ,Structure , spectrum , resistance , Side effect ,
-Drugs :
1-imipenem/Cilastatin Amp 0,5
2-Ertapenem 0,5 amp
-Structure : uniq changes in the structure, Containing B-Lcatamse ring
-Spectrum: broad spectrum duo to :
1-Gram +
2-Gram -
3-Pusdomonas
4-Anearobic
—Resistant : highly resistant
-Side effect : the imipenem alome cause nephrotoxcicty from its products by enzyme Dyhdryopeptedase , So we administered with Cilastatin inhibits the renal dyhdryopeptadese to prevent formation of toxic formation
-Etrapenem : its without this effect so administered alone
Explain glycopeptides ,Drug , mechanism,spectrum,Pharmcokintics ,side effects uses
-Drug : Vancomycin Amp 0,5 iVI
-mechanism: inhibits cell wall synthesis by binding to D-Ala-D-Ala terminal of growing peptide chain during cell wall synthesis resulting inhibitions of the transpeptdese reaction , Prevent further elongation and cross - linking of peptidoglycan
-Spectrum : narrow spectrum duo to :
Only gram + such as :
1-Staphylococci MRSA
2-P.Cocci
3-Entra cocci
4-Anearobic infeaction
-Pharmcokintics:
1-Not absorbed orally
2-Not metabolise in liver
3-Execreted by kidney
-Side effect :
1-Red man syndrome: Histamine reales
2-Nephrotoxcicty
3-Ototoxicity
4-Vein thromphlitis
—Uses :
1-MRSA
2-Culstrirudum diffucel colitis
classification of protines synthisis antibiotics
a) Antibiotics targeting the 50S ribosomal subunit
macrolides
lincosamides
chloramphenicol
б) Antibiotics targeting the 30S ribosomal subunit
aminoglycosides
tetracyclines
Explain The Proteins synthesis Inhibitors ( Aminoglycosieds ) Drugs , chemistry , Pharmcokintics, Mechanism of Action , resistance, Spectrum, Uses , adverse effects
-Drugs :
1-Streptomycin Pwdr 1st gen
2-Gentamicin amp 2gen
3-Amikacin pwdr 3 gen ( synthetic drug)
-Chemistry : Consists of NH2+ amino group and glycoside : sugar , And hydroxyle group which is mean ita water sulable
-Pharmacokinetics:
1-Absorption: not orally duo to inozed charge
2-Distribution:
2-1 Not Pass BBB , but pass placenta and its tetaroginic , breast milk Pass ( and its not tetarogenic ) bcs its not absorbed orally
3-Metabolism: in liver
4-Excretion : kidney, high concentration and unchanged and increases alkalinity of urine , Normally Ph of urine is 5.8 so the drug are more used in alklain urine which is needed to treat UTI
—Mechanism of action :
-its inhibit the protein synthesis by binding irriverasbly in the 30s subunit ribosome , which lead to error in the mRNA reaching and formation of functional abnormal proteins
-In details it consists of 3 phases :
1-Attachment: which the amino group NH2+ have positive charge , there will be attraction (Electrostatic Attraction ) bcs the outer membrane of the gram - its consist of negative charge
2-open pores : the outer membrane pores will open only incase of needed of nutrients and the aminoglycosides are similar to the nutrients so the pores will open and the drug molecules will enter
3-irreversible bond : once the drug reached the nucleus there is the ribosomes 30s subunit and it will bind to it irreversibly and inhibit mRNA translation
-Spectrum: they are bactriocidal ( broad spectrum shifted towards Gram -) duo to :
1-Mainly gram - : Entrobactria , Pusdomonas (2gen ,3gen ) , mycobacteria ( 1gen , amikacin )
2- few gram + : staphylococcus
3-TB
-Resistant:
1-P,Coccai
2- Anearobic and intercellular pathogen such as. (Calm my leg )
3-Cant be used for acquired
resp infection
-Uses :
1-Gram - infection: E coli UTI
3-Resp infection
4-Gram - spetecymi
5-TB : Streptomycin , Amikacin
-Side effect :
1-Neohrotoxcity : duo to exacration of this drug in renal , and bcs has + charge and can bind to Kidneys proteins
-VIP-2-Nerve toxicity 8th cranial : the molecule of this drug enters the inner ear and cause toxicity to the 8th cranial nerve ( vitebular and auditory ) and cause deafness duo to accumulate in the endolymph of the inner ear
-VIP-3-NMB : muscle weakness, we can reverse it with Neostagmine
—Dosage : 5mg per kg and its concentration killing dependent
Explain The Proteins synthesis Inhibitors ( tetracycline) Drugs , chemistry , Pharmcokintics, Mechanism of Action , resistance, Spectrum, Uses , adverse effects
-Drugs :
1-Tetracycline Tab
2-Doxycycline tab/pwder
—Chemistry : there MW less then 500 , and they consist of hydroxyl group which is mean they are water sulable
-Pharmcokintics:
1-Absorpation : incomplete duo to water sulablety , food decrease teh absorption and they are make complex with the metals ( doxycycline is more absorbed)
2-Distribution:
2.1 BBB : not pass
2.2 Placenta / breast milk :pass and its teratogenic
2.3 body fluids :reach
3-metabolism: liver , and exctinssive metabolism , duo to entrohepato circulation
4-Execration : mainly kidney , but they cant Treat UTI duo to extansive metabolism in liver and the drug becomes inactive , but doxycycline’s 50% renal and 50% bilary which can use with patient with renal impairment, but in the same time they are hepatotoxic duo to entroheptaic circulation
-mechanism of action :they are binding reversiblly to 30s subunyand inhibiting the binding of Aminoacyl-tRNA to The Aminoacyl-Centre which is lead to disrupting the early stage of translocation-imitation
-spectrum: broad spectrum/ bacteriostatic
1-most G+ but not Staph
2-most G- but not pausdomonas
3-most of Anearobic bacteria ( CL difesil )
4-Atypical organisms ( Calm my leg ) + borrlia , Reckissia , Coxilla
5-Protozoa : malaria , Toxoplasma ( bind to 40s )
-Resistant: Cross resistant easily and rapid
-uses :
1-Sexual transmitted infections : in patients who has tolerance to B lactamse
2-Pneumophil ( Ligunla )
3-peptic ulcer
4-dangerous infection; Plague , cholera , Antha
4-Zoomases ( loptosorosis , bracellosis )
5-Intracellular pathogens: such as lyma disease, Ricksosis , Q fever )
6-Acne
-Advera effect :
1-GIT upset
-VIP-2-teeth and bone : ditrubunce of skeleton formation deposition in bone and teeth leading leading to ( Colouring the enamel in yellow-Brown color )
-VIP-3-Cholistatic hepatitis: liver cell injury, hepatotoxic, Hypertophy of the hepatocyte
-VIP-4-Photosensitivity
-C.I :
1-Allergies from tetracycline
2-Children under 8 years
3-Pregnancy
4-Liver impairment
Explain The Proteins synthesis Inhibitors ( macrolides ) Drugs , chemistry , Pharmcokintics, Mechanism of Action , resistance, Spectrum, Uses , adverse effects
-Drugs :
1-Erythromycin tab/pwdr 1gen
2-Clarithromycin tab/pwdr 2gen
3-Azithromycin tab 2gen
—Chemistry : consists of macrolacton ring , and sugar and its MW more then 500
-Pharmcokintics:
1-Absorpation : poor and deceased by food
2-Distribution:
2.1 BBB : not pass
2.2 Placenta / breast milk : pass and they are not teratogenic
2.3 body fluids : they reach most body fluids with good concentration ( they have selective distribution to neutrophils and phagocytes
3-metabolism: in liver
4-Execration : they are execrated through liver billary and entrohepatic circulation, thats why they are heptao toxic,
-NB! 1gen is not stable in acid stomach so low bioavailability and short half life , 2nd generation is the opposite
-mechanism of action : they bind reversible to 50s subunits of the ribosomes and inhibit peptide transferase , and inhibit elongation of proteins, which block the translocation of ribosomes to the next Codon on the mRNA
-Spectrum: Bacteriostatic / Concentration dependent, Spectrum:
1-Mainly G +
2-Intercellular pathogens: Calm my leg
3-H.Pylori : Clarithromycin
-Resistant: in the case id macrolides the bacteria becomes resistant in approximately 10 days by changing the 50s binding site
-uses :
1- Gram +
2-Atypical organisms
3-otaits media
4-sinuses
-Advera effect :
1-GIT upset
-VIP-2-Cholistatic hepatitis: duo to accumulation in liver entrohepatic circulation, inhibitory of CYP450
-VIP-3- Ototoxcity
-VIP-4-Prolongation of QT interval : which could cause a ventricular arrhythmia
-C.I : combination of macrolides and penicillins
