Control-Find whatever antbiotic you’re interested in to learn unique facts about it (or scroll for memes)!

Shayne McKee Pharmacy Antibiotic Meme

Natural Penicillins (Pen VK, Pen G, Pen G Procaine/Benzathine/Procaine & Benzathine)

Penicillin VK and Penicillin G

- Pen G: Unstable in gastric juice (pH 2), thereby limiting absorption (IV only)

Pen VK: More stable, higher serum concentrations

Short T1/2, Renal elimination (tubular secretion)

Removed by hemodialysis

Bactericidal compounds. Maximal activity is based on TIME ABOVE MIC

Concentrations must be above MIC for 50% of the time for maximal effectiveness (30% for stasis).

Spectrum

Oral anaerobes (but not gut anaerobes like bacteroides/fusobacter)

Gram positives

Strep & Strep pneumoniae

Viridans strep

E. Faecalis, but not faecium

Neisseria.

Treponema pallidum (Syphilis)

DO NOT cover MSSA/MRSA

Indications

Primarily syphilis

Others:

Endocarditis

Meningitis

Strep pharyngitis

Streptococcal toxic shock

Penicillin G Procaine (Long acting parenteral)

IM
Absorbed over about 2-4hrs
Challenges associated with this drug:
- Requires daily administration
- Neisseria were resistant
May cause dizziness

Shayne McKee Pharmacy Antibiotic Meme

Penicillin G Benzathine (Long acting parenteral)

IM
Drug remained in serum for up to 4 weeks!
Challenge: severe joint pain

Penicillin G Benzathine/procaine (Long acting parenteral)

IM
LESS painful than benzathine

Antistaphylococcal Penicillins (Oxacillin, Nafcillin, Dicloxacillin)

Oxacillin & Nafcillin

Spectrum:
- Gram positives
  - Strep & S. pneumo
  - Viridans strep
  - MSSA but not MRSA
IV ONLY – gastric acid causes breakdown
Short T1/2
Hepatic & Biliary excretion
Distribute into multiple tissues (skin/joint/lung/urine/CSF [with inflammation]), bile, peritoneal cavities
May cause increased transaminases – more likely in these two drugs because their elimination is hepatic

Dicloxacillin

ORAL!
- Increased F compared to oxacillin and nafcillin
Still have a short half-life
Used for mild SSIs
Again, covers MSSA but not MRSA

Extended-spectrum Penicillins

Aminopenicillins (Ampicillin, Amoxicillin, Amp/Sulbactam, Amox/Clav)
Ureidopenicillins (piperacillin/tazobactam)

Ampicillin

Has enhanced cell wall penetrating capability due to being a zwitterion at neutral pH. This allows them to easily penetrate through a gram negative cell’s porins.
Absorption is SATURABLE. Increasing dose does not produce greater effect. Higher doses lead to more diarrhea (this drug’s main problem).
Penetrates lung, bone, CNS.
Used empirically in Listeria infections (esp. CNS)

Amoxicillin

Oral ONLY
Reduced diarrhea vs. ampicillin
Primary use is for upper respiratory tract infections
- Used empirically against S. pneumo (high dose)

Ampicillin/Sulbactam

IV only (2 ampicillins: 1 sulbactam)
Minimized impact of beta-lactamases, penicillinases, and cephalosporinases.
Sulbactam is a “suicide inhibitor”
- Permanently inactivates beta-lactamases. Cannot be reused.
Sulbactam has weak activity against Neisseria and Acinetobacter
Both have short T1/2, renal elimination.
Sulbactam penetrates CSF, lung, and bone similar to Ampicillin.
Empiric uses:
- Surgical prophylaxis for intra-abdominal surgery
- Head and neck infections involving the oral cavity
- Sinus infections
- MDR Acinetobacter infections
Definitive uses:
- Intra-abdominal, head and neck infections, and gynecologic infections

Amoxicillin/Clavulanate

Only available in ORAL formulations

Suicide inhibitor

Inhibits beta-lactamases

In contrast so sulbactam, no activity against Acinetobacter

While amoxicillin is renally eliminated, clavulanate is eliminated by renal & hepatic mechanisms.

Primary complaint is diarrhea.

Primary use is in upper respiratory infections:

Sinusitis

Otitis media

Strep throat

Penicillin/tazobactam

IV only
Short T1/2, renal elimination
Extensive distribution into bile, CNS, lung, skin, urine, bone, peritoneum
The only thing it does not cover is MRSA
More likely to cause cholestatic jaundice than other beta-lactams
Uses:
- Healthcare infections where MDR is suspected
- Intra-abdominal infections
- Pneumonia
- Complicated skin/skin structure infections
- Fever/neutropenia

Shayne McKee Pharmacy Antibiotic Meme

Cephalosporins

1st : Cefazolin, Cephalexin, Cefadroxil

Cefazolin & Cephalexin & Cefadroxil

Cefazolin: IV ONLY! The only 1st gen with poor F

Cefazolin has unique use in surgical prophylaxis

Short T1/2, renal elimination

CSF penetration = POOR. Can’t be used for CSF infections. Active efflux from BBB.

Good penetration into skin, bone/joint, urine, and lung (variable)

1st gens do not cover strep pneumo.

Uses:

SSIs; MSSA; S. pyo/Agalactiae

UTIs; E. Coli

Definitive therapy for MSSA (cefazolin)

2nd: Cefprozil, cefaclor, cefuroxime, Cefotetan, Cefoxitin

Cefprozil, Cefaclor, Cefuroxime, Cefotetan, Cefoxitin

Bioavailability: Good for all except Cefotetan and Cefoxitin

These are both IV ONLY

Cefotetan has the longest half-life

Both of these agents have anaerobic activity and are used as intra-abdominal agents

All are renally eliminated

Cefprozil has the lowest renal elimination

Still struggle with CSF penetration

2nd gens can be broken down into respiratory and cephamycins

Respiratory:

Cefprozil

Cefaclor

Cefuroxime

Cephamycins (just remember that they’re the IV forms)

Cefoxitin

Cefotetan

They cover the same things except cephamycins cover anaerobes.

Respiratory cephalosporin uses:

Upper/lower respiratory infection

Otitis media

Cephamycin uses:

Intra-abdominal infection

Mycobacterial infection (cefoxitin)

Surgical prophylaxis

Cefotetan may cause a disulfiram-like reaction

3rd: Cefixime, cefdinir, cefpodoxime, ceftriaxone, cefotaxime

Cefixime, cefdinir, cefpodoxime, ceftriaxone, cefotaxime

Cefixime: Used for gonorrhea management
Ceftriaxone and Cefixime: Longest 3rd gen half-lives
- 🡪 Once daily dosing
All have pretty low renal clearance so it is less likely to have to adjust for renal dysfunction (biliary cleared as well)
What we’ve been waiting for.. CSF penetration!
NO activity against ESBL and POOR activity against AmpC
Unlike 2nd gens, they lose activity against gut anaerobes like bacteroides
NOT ideal for MSSA – first and second gens are BETTER
Uses:
- CNS infections
- Upper/lower resp tract infection
- Otitis media
- UTIs
- Bone/joint
- SSIs
- Intra-abdominal infections
More frequent CNS side effects due to their CSF penetration abilities
- Seizures
- Confusion
- Delirium
More frequent diarrhea because 3rd gens are the only cephalosporins with biliary elimination
Ceftriaxone is contraindicated in neonates <28 days (hyperbilirubinemia)
- Ceftriaxone binds with calcium, forming Ringer’s lactate solution
- Biliary sludging and nephrolithiasis may occur.
Cefdinir should be taken separate from iron supplements 2 hours before or after dose.

Antipseudomonal and Antistaphylococcal Cephalosporins

Antipseudomonal: Ceftazidime, Cefepime, Ceftazidime/avibactam, Ceftazolane/tazobactam
Anti-staphylococcal (anti-MRSA): Ceftaroline

Ceftazidime

Activity against Achromobacter and stenotrophomonas, which is not seen with other members of the 3rd gen family
UNSTABLE against ESBL and AmpC
Ceftazidime should not be used for gram-positive infections.
Covers every gram-negative except Acinetobacter. Because of its instability against AmpC/ESBLs, it is not ideal against species like Enterobacter/Citrobacter/Serratia.
Poor activity against B. fragilis
Can penetrate CSF with inflammation

Cefepime

POOR activity against Achromobacter and stenotrophomonas.

STABLE against AmpC

Better gram-positive coverage (up to MSSA); PREFERRED for gram (+) over ceftazidime

Some activity against Acinetobacter

Ceftazidime/Avibactam

Avibactam allows for inhibition of ESBL, AmpC, KPC and OxaA
- Avibactam is a non-suicidal inhibitor and can be recycled.
As with ceftazidime, still not ideal for gram positives.
Much better coverage against ESBL producing bacteria (Enterobacter, Citrobacter, Serratia, P. aeruginosa) than ceftazidime alone
- Although it does have activity against ESBL/AmpC, its activity is not better than carbapenems
Predominant use in KPC-producing organisms

Ceftolozane/tazobactam

Similar to other anti-pseudomonal cephalosporins BUT it has greater activity against Pseudomonas aeruginosa.
- It is active against carbapenem-resistance pseudomonas.
Use for P. aeruginosa infections (especially for carbapenem-resistant isolates)!

Ceftaroline

Ceftaroline is the active metabolite. Ceftaroline fosamil is the prodrug that gets converted to active ceftaroline by phosphatases.
ACTIVE against MRSA (anti-staph/anti-MRSA agent)
NO activity against ESBL and poor activity against AmpC
- Loses activity pseudomonas/acinetobacter and reduced activity against Citro/Entero/Serratia
Used in pneumonia, bacteremia, SSIs
ADEs
- CNS: seizures, confusion, delirium
- GI: N/V/D
- Renal: interstitial nephritis
- Anaphylaxis: CROSS REACTIVITY with PCN allergy. DO NOT USE in patients with immediate onset reactions (anaphylaxis)
- Hematologic: neutropenia, anemia, thrombocytopenia, False positive Coombs test

Carbapenems (Imipenem/Cilastatin, Meropenem, Doripenem, Ertapenem)

Anti-pseudomonal carbapenems: Imipenem/Cilastatin, Meropenem, Doripenem

Cilastatin used with imipenem to inhibit DHP1, an enzyme that degrades imipenem
Meropenem and Doripenem have a methyl group that blocks DHP1 hydrolysis and can be used without cilastatin.
Meropenem and Doripenem have reduced epileptogenic potential (seizures)
CSF penetration! (greatest in meropenem)
Of the beta-lactams, they require the shortest amount of time above the MIC to work effectively.
These drugs cover everything except MRSA, E. faecium, and Stenotrophomonas. That is why they’re nicknamed “Gorillacillin.”
They are all stable against ESBLs and AmpC
- Because of this, they have a tendency to select for resistant bacteria and are usually reserved as a last line of defense when other anti-pseudomonal drugs like Cefepime or Pip/tazo fail or there is clinical worsening while taking these medications.
Potency in order: Doripenem > meropenem > imipenem
All carbapenems (inc. ertapenem) interact with valproic acid and probenecid.

Ertapenem

This drug DOES NOT COVER:
- Pseudomonas
- Acinetobacter
- E. faecalis
- E. faecium
  - Why??
    - Its structure has anionic character that results in decreased penetration through the porins of gram-negative bacteria.
What’s its use then?
- It stands out because of its half-life. It requires only once daily dosing.
  - Eases transition to home care
Like the other carbapenems, is it is stable against ESBL and AmpC and inactive against S. maltophilia.

Shayne McKee Pharmacy Antibiotic Meme

Monobactams (Aztreonam)

ONLY active in gram-negative bacteria. Aztreonam

- Not active in Neisseria or Acinetobacter
While the same MOA as other beta-lactams (binding PBPs), it has a specific high affinity to PBP-3. PBP-3 is a septum peptidoglycan transpeptidase used in cell division.
- Bactericidal; time dependent killing; T>MIC of at least 50% required
Short half-life, renal elimination
Administered IV, IM or Inhaled
POOR eye penetration and POOR CSF penetration without inflammation
Requires renal adjustment
ACTIVE against Metallo-beta-lactamases (S. maltophilia) but INACTIVE against ESBLs and AmpC
- Main mechanism of resistance to aztreoname is hydrolysis by beta-lactamases
CAN BE USED in patients with penicillin allergy
Can also be used in combination with another beta-lactam when an aminoglycoside or fluoroquinolone is not appropriate.

Aminoglycosides (Neomycin, Kantamycin, Gentamicin, Tobramycin, Plazomicin)

Shayne McKee Pharmacy Antibiotic Meme

Neomycin, Kantamycin, Gentamicin, Tobramycin

AG’s are NUCLEOPHILIC molecules that can easily be inactivated by transferring their own electrons – makes them an easy target for modification enzymes
Unique membrane penetration
- AG’s must pass through the outer membrane and the cytoplasmic membrane.
  - To get through the outer membrane, AG’s create porins that induce their uptake with Mg (II) bridges.
  - They then diffuse through the periplasmic space where they encounter the cytoplasmic membrane
    - They get through the cytoplasmic membrane via energy-dependent phase I (requires electron transport)
Mechanism of action
- Inhibits protein synthesis
- Elicits premature termination
- Incorporates incorrect amino acids
Activity of aminoglycosides are impacted by acidic pH, anaerobic conditions, hyperosmolarity, and divalent cations.
IV only, renal elimination
- Elimination is Tri-phasic
  - Alpha, beta, and gamma phases.
    - Alpha – distribution of drug from blood to tissue
    - Beta – elimination through kidney
    - Gamma – slow release of drug from binding sites (kidneys, ears)
GOOD penetration into bone, synovial fluid, and urine
POOR penetration into bronchial secretions, CNS (EVEN in inflamed conditions), eyes, bile, prostate and purulent fluid.
Concentration dependent killing
- Cmax/AUC: 8-10
- AUC:MIC: >100
Always keep trough values <2mcg/mL to minimize toxicity
AG therapy should be ONCE DAILY to minimize toxicity.
AG’s are ACTIVE against mycobacteria, and many gram positives and negatives. However, they are almost never used as monotherapy and always as combination therapy, especially in deep-seated gram-positive bacteria (endocarditis or device-related infections).
- An exception is that an AG could be used as monotherapy with a UTI
Resistance
- Enzymatic modification is most common and is plasmid mediated.
- Decreased uptake mechanisms are chromosomally mediated and usually cross-resistant to AG’s
Adverse effects
- NEPHROTOXICITY
  - Non-oliguric renal failure (continues to produce urine)
  - A slow rise in serum creatinine is seen along with changes in urine input/output, and sometimes proteinuria.
  - After several days of therapy, the AGs accumulate and cause epithelial cell necrosis 🡪 nephrotoxicity.
- OTOTOXICITY
  - Irreversible vestibular and auditory effects
    - Can occur during or after the end of therapy
    - Can occur with standard dose or once daily dosing (equal risk); there is NO SAFE DOSE.
    - There is no correlation between peak or trough concentrations, but increased risk with sustained high trough concentrations
    - There is no relationship between serum AG and levels within the inner ear.
    - Usually high frequency hearing loss goes first and may not be recognized clinically. Low frequency hearing loss shows loss in conversational hearing.
    - GENTAMICIN most vestibulotoxic.

Plazomicin

Active against aminoglycoside-resistant isolates (aminoglycoside modifying enzymes)
Active against ESBLs
Active against carbapenem-resistant Enterobacteriaceae
Has a prolonged post-antibiotic effect
Has less gram-positive activity than the other aminoglycosides
Plazomicin is ACTIVE against gentamicin-resistant Enterobacteriaceae, but activity is POOR against gentamicin-resistant Pseudomonas
Like aminoglycosides, not active against Stenotrophomonas
Like other AG’s, dose is adjusted for impaired renal function
Therapeutic drug monitoring: Cmin <3mcg/mL in patients with UTI
Nephrotoxic effects do occur, but tend to occur less. They occur more often with CrCl <60mL/min and high concentrations where trough values are >3mcg/mL
Ototoxic effects not observed, but monitor closely.

Glycopeptides (Vancomycin)

Shayne McKee Pharmacy Antibiotic Meme

Vancomycin

Available as IV or Oral

Exclusively a gram-positive agent:

Staph (MSSA/MRSA), S. epidermidis

Strep

Enterococcus (Faecalis ONLY)

Corynebacterium

Listeria

Bacillus

C. diff (Oral formulation ONLY)

The oral form is not absorbed and concentrates in the GI to kill C. diff.

If using more than 2g/day for >10 days, requires therapeutic drug monitoring

Gram positive oral anaerobes (peptostreptococcus)

MOA:

Inhibits peptidoglycan synthesis by recognizing D-alanine-D-alanine bonds, and binding to them. Cell wall cannot form.

CSF penetration depends on if meninges are inflamed or not.

Decent lung penetration – enough to kill most bacteria.

DOSING:

Empiric: 15mg/kg IV q8-12h, use actual body weight

Critically ill: loading dose of 25-30mg/kg to achieve SS faster

Vancomycin requires therapeutic drug monitoring

Trough goal should be about 15-20mcg/mL

Check the trough prior to the 4th dose

Red-Man Syndrome

A histamine-like reaction that will present with flushing, tachycardia, warmness, a rash on the face/upper body area, but NOT associated with an allergy.

It occurs due to rapid infusion of vancomycin.

Aim to infuse at <10mg/min

Consider co-administrating with antihistamines

Pregnancy category B.

No (few) drug interactions

Vancomycin is concentration dependent

Estimate AUC: Total vancomycin dose in 24h / clearance

Goal AUC/MIC to maximize killing: 400mg/L

More frequently used equivalent is a trough goal of 15-20mcg/mL

Resistance

Van A gene will change D-alanine-D-alanine to D-alanine-D-lactate, so vancomycin won’t recognize the bond.

Results in VRE

Staph aureus can pick up the van A gene via plasmids

Results in VRSA

Lipoglycopeptides (Telavancin, Dalbavancin, Oritavancin)

Telavancin

Dual MOA – it acts at the cell wall and cell membrane
- 1) Same as vancomycin – interacts with D-ala-D-ala bond at the cell wall (peptidoglycan)
- 2) Hydrophobic tail penetrates cell membrane, causing it to depolarize and increases its permeability
FDA approved for HAP and VAP
MORE potent than vancomycin for MRSA and MSSA
ACTIVE against VRE Enterococcus that have VanB (NOT vanA)
Co-formulated with Hydroxyl-propyl-Beta-cyclodextrin to enhance solubility
Renal elimination
- Renal adjustment required. Do not use if CrCl <10mL/min
- Cure rates decreased for ABSSSIs with CrCl <50mL/min
- Watch for renal adverse events/SCr increases
ADEs
- Taste disturbance (metallic/soapy taste) most common
- CONTRAINDICATED in pregnancy
- CONTRAINDICATED with heparin
- Caution using other QT-prolonging agents
- Can prolong aPTT for up to 18 hours (interferes with phospholipid agents used in measuring thromboplastin time/prothrombin time, as well as interfering with coagulation-based factor X assays)

Long-acting Lipoglycopeptide: Dalbavancin

Use: ABSSIs
Gram-positive activity
- VanB and VanC VRE (not Van A)
- MRSA/MSSA
- Great for gram-positive anaerobes
- 2 week half-life! – once weekly dosing (or twice)
  - Serum concentrations can stay above MIC for over a month
- Reconstitute with ONLY WATER or 5% dextrose
- Administer over 30 minutes
- Rapid infusion -> red man syndrome
- N/D/Ha
- No drug-drug interactions

Shayne McKee Pharmacy Antibiotic Meme

Long-acting Lipoglycopeptide: Oritavancin

- MOST potent of vancomycin, dalbavancin, linezolid, etc.

ACTIVE against VanA

ACTIVE against VISA/VRSA

Half-life 8-10 days

Renal elimination, but does not require renal adjustment because it is cleared very slowly.

ONLY administer with 1000mL of D5W

Monitor patients with CHF because of such a large volume of fluid

ONLY administer over 3 hours

Artificially prolongs aptt up to 120 hours

Artificially prolongs INR and PT (prothrombin time) for 12 hours

Monitoring warfarin effectiveness unreliable

Most common ADE:

N/V/D/Ha

Limb or subcutaneous abscesses

MONITOR patients for osteomyelitis (more cases reported in oritavancin than vancomycin)

Uses of Dalbavancin/Oritavancin

Avoiding hospitalization because of their long half lives that can remain in plasma for over a month

Minimizing extended hospitalization stays

Preventing need for multiple IV therapies

Could help with compliance with those unable to maintain IV access (e.g. homeless)

Daptomycin (a lipopeptide)

Daptomycin

Bactericidal
FDA approved for:
- Complicated SSSIs
- Staph. Aureus bloodstream infection
- Right-sided endocarditis caused by MSSA/MRSA
Does NOT cover pneumonia
Does NOT cover left-sided endocarditis
POOR CSF penetration
Unique MOA:
- Lipid tail inserts itself into the membrane (calcium mediated)
- Causes membrane to depolarize
- Ions (K+) efflux out of the cell, inhibiting protein and other macromolecule synthesis
- 🡪 Cell dies, but the cell does not rupture
  - Less of an immune response is elicited as a result
Spectrum is only gram-positive:
- MSSA/MRSA
- Enterococci (VRE)
- Strep
- Gram-positive anaerobes
Renal elimination – consider monitoring SCr
Dosage is based on CrCl and the type of infection
- Duration of treatment for cSSSI: 7-14 days
- Duration of treatment for S. aureus bacteremia: 2-6 weeks
- Higher doses needed for enterococci and persistent bacteremia
ONLY administer in 0.9% NaCl (NS) – not compatible with dextrose diluents
Must infuse at 30 minutes or inject (IV Push) in 2 minutes
Adverse effects and warnings:
- Most common ADEs are N/D/C/Ha
- Warnings:
  - Rhabdomyolysis or myopathy
    - Monitor CPK levels at baseline and weekly thereafter
    - Monitor or hold for patients taking HMGCoA reductase inhibitors
    - Discontinue daptomycin if myopathy is present and CPK is > 5X normal (1000 U/L)
    - Discontinue daptomycin if patient is asymptomatic and CPK is 10X normal (2000 U/L)
  - Eosinophilic pneumonia
    - Occurs 2-4 weeks after starting daptomycin
    - Improves with discontinuation and steroid therapy
    - Suspect eosinophilic pneumonia in patients with fever, hypoxia, or pulmonary infiltrates
No drug interactions
Daptomycin can cause false prolongation of INR and PT with some thromboplastin reagents.
Resistance in Enterococci and S. aureus:
- Mediated by dltA gene
  - Causes changes in cell membrane permeability; cell membrane has less affinity for daptomycin
- Mutations in genes associated with phospholipid synthesis

Oxazolidinones (Linezolid, Tidezolid)

Linezolid

BacterioSTATIC
Linezolid binds inhibits protein synthesis by binding to the 50s ribosome peptidyl transferase center (PTC; the 23s rRNA) and stopping the growth of bacteria. Blocks the formation of 30S and 50S ribosome complex.
The acetamide group of linezolid causes a reduction in its activity
Spectrum is gram-positive
- MSSA/MRSA
- Enterococcus (VRE)
- Strep
- Gram-positive anaerobes
- Mycobacterium and Nocardia
FDA approved for:
- VRE
- Nosocomial and CA pneumonia
- Uncomplicated and complicated SSSIs
IV and PO both have 100% F
NO renal or hepatic adjustment needed
GOOD CSF penetration
Adverse events:
- Myelosuppression
  - Thrombocytopenia > anemia > neutropenia
  - Usually happens after > 2 weeks of use
  - Perform a weekly CBC
- Optic neuritis with use >28 days
- Peripheral neuropathy with use > 28 days
Interactions:
- None, but can act as an MAOI inhibitor
  - May interact with serotoninergic agents, MAOIs, and tyramine-containing foods
  - May cause serotonin syndrome within 6 hours of use
    - Mental status changes, hyperreflexia, shivering, fever, diarrhea, tremors
Resistance:
- Mutations of the 23s rRNA (the portion of the 50S that binds the 30S subunit)
- cfr gene can cause resistance in Enterococci and Staph. aureus

Tedizolid

A PRODRUG
A phosphate modification increases solubility, bioavailability, and limits the reaction with MAOIs
- When this phosphate is cleaved and replaced by an OH group, it remains active against cfr genes!
Tedizolid has two extra rings that allow tighter binding (greater potency) to the PTC (the 23s rRNA) of the 50s subunit.
Same MOA as linezolid – prevents translation of proteins.
Used for ABSSSIs; treatment duration 6 days
More potent than linezolid in every way and retains activity against linezolid-resistant MRSA
Like linezolid, bacteriostatic and 100% F, and NO adjustments for renal or hepatic impairment
Possibly WEAKER interaction with MAOIs than linezolid
- Evidence is lacking since they excluded patients taking MAOIs in their trials
Most common ADE is Nausea
Tidezolid RETAINS ACTIVITY against VRE and linezolid-resistant MRSA that have the cfr gene

Tetracyclines and Glycylcyclines

Tetracyclines (Tetracycline, doxycycline, minocycline, Eravacycline, Omadacycline)
Glycylcyclines (Tigecycline)

All tetracyclines

BacterioSTATIC
NONE have activity against Pseudomonas
Entry into cell and MOA:
- Gram-positives: Enter via pH-dependent active transport
- Gram-negative: Enter via porin channels
- Inhibits protein synthesis and elongation by acting on the 30s subunit
Active against various atypicals like parasites/spirochetes
ADEs:
- GI side effects: N/V/D/Heartburn/Epigastric pain
- Photosensitivity & Hyperpigmentation
  - Blue-black discoloration occurs in scars/inflammation
  - Muddy-brown pigment occurs on sun-exposed areas
    - Use sunscreen and protective clothing
- Teeth can become yellow/gray/brown; permanent
- Bone growth can be inhibited in infants/children under 8 y/o
  - Reversible
  - Avoid use
- Nephrotoxicity
- Neurotoxicity
  - Neurototic effects seen more in minocycline (dizziness, vertigo, tinnitus) and these effects are seen more often in women
  - Pseudotumor cerebri can also occur (high pressure that develops in brain and mimics a tumor)
- AVOID IN PREGNANCY – can cross placenta and have toxic effects on fetus (retard skeletal development) – this effect goes hand-in-hand with its other bone growth inhibition effect.
Reduced risk of C. diff infection
Interactions:
- CATIONS (di/trivalent) reduce absorption
  - Take 1-2 hours before or 2 hours after
  - Buzz word: multivitamin
- Oral anticoagulants:
  - Increase bleeding risk by decreasing vitamin K production
- Oral contraceptives
  - Reduce birth control drug levels
    - Use mechanical means of contraception in addition to BC

Tetracycline

IV formulation no longer available due to hepatotoxicity
AVOID IN RENAL IMPAIRMENT
Can cause hepatitis
All tetracyclines have a long half-life except Tetracycline
HIGHEST renal elimination
TAKE ON AN EMPTY STOMACH, food reduces absorption 50%

Doxycycline

- IV and PO
- 100% F
- SAFE in renal impairment due to high fecal excretion
- Does NOT cause hepatitis
- ADEs:

Pill esophagitis

- - Take with 8oz water and stay upright for 30 minutes
Carbamazepine, phenytoin, and barbiturates DECREASE half-life of doxycycline, thus decreasing its therapeutic effect.

Minocycline

IV and PO
100% F (slide says 90% to be specific, but IV and PO conversions are 1:1)
Does not need renal or hepatic adjustment
LOWEST fecal elimination
ADEs
- Long-term use of minocycline can cause blue-black gum discoloration due to bone pigmentation under the gums

Tigecycline (Glycylcycline)

Steric hindrance allows tigecycline to overcome efflux pumps and ribosomal protection
Most common ADEs: Nausea/Vomiting
NO dosage adjustment in renal impairment
Adjust for severe hepatic impairment: 25mg IV q12h vs typical 50mg IV q12h
DO NOT USE for bloodstream infections/bacteremia
- Drug’s Vd is high and binds tissues very well – leaving serum concentrations very low
Uses:
- CAP
- Complicated intra-abdominal infections
- Complicated skin and skin structure infections
WARNING:
- Mortality was HIGHER with tigecycline use. Only use when no other alternatives are available
Resistance to Tigecycline:
- Tet genes – plasmid mediated
- Efflux pumps (gram positive and negative)
- Ribosomal protection proteins

Omadacycline

IV or PO
LOWEST renal elimination
LOWEST protein binding
Uses:
- CAP
- ABSSSIs
ADEs:
- Transaminitis, hypertension, insomnia, gastrointestinal upset

Eravacycline

Use: Complicated intra-abdominal infections
If using a strong CYP3A inducer concomitantly, Eravacyline’s clearance is increased.
- UP DOSAGE to 1.5mg/kg q12h
DO NOT USE Eravacycline for complicated UTIs
- In clinical trials it did not show statistical non-inferiority vs Ertapenem

Sulfonamides (Bactrim)

TMP/SMX (Bactrim)

- Sulfonamides are analogs of PABA
  - Competitively inhibits dihydropteroate synthase, reducing dihydropteroic acid concentrations
- Trimethoprim inhibits dihydrofolate reductase, reducing tetrahydrofolate concentrations
- Almost 100% F
- Available as oral/oral suspension/IV
- Dosage depends on the infection
  - Dosage is based on trimethoprim component
  - Use adjusted bodyweight for obese patients
- ADJUST for renal dysfunction
- TMP/SMX is FIRST LINE for:
  - Nocardia
  - Stenotrophomonas maltophilia
  - B. cepacian
  - Pneumocystis jiroveci
- Covers MSSA/MRSA
  - Beta-lactams more effective for MSSA
- Does NOT cover Pseudomonas or enterococcus
- NO anaerobic or atypical coverage
- Resistance:
  - Permeability barriers/efflux
  - Altered binding to dihydrofolate reductase (trimethoprim)
  - Altered binding to dihydropteroate synthase (sulfonamides)
  - Resistance can be transferred to other organisms

- Pregnancy category D

- ADEs

- - Most common side effects are GI related: N/V/D/Anorexia

- - Hyperkalemia can be caused by TMP (it has a potassium-sparing effect)

- - Increased SCr from TMP, but filtration is not affected

- - Interstitial nephritis or crystalluria from sulfonamide

- - Interactions

- - TMP:

- - Dofetilide

- - Phenytoin

- - Warfarin

- - Digoxin

- - SMP:

- - Nephrotoxic agents

- - Methenamine – Avoid

- - Elvitegravir

- - Sulfadiazine (a different drug than TMP/SMX) is used for toxoplasmosis

Fluoroquinolones (Ciprofloxacin, Levofloxacin, Moxifloxacin, Gemifloxacin, Delafloxacin)

Ciprofloxacin

Shayne McKee Pharmacy Antibiotic Meme

Of the fluoroquinolones, it has lower F than most (except Delafloxacin)
Of the fluoroquinolones, its half life is the lowest (along with Delafloxacin) – needs BID dosing vs. once daily for others.
Renally eliminated
Think gram-negatives (Pseudomonas included)
Cipro specific drug interactions (due to its CYP1A2 inhibition potential):
- Theophylline – increases levels. AVOID concomitant therapy
- Cyclosporine – increases levels
- Methotrexate – inhibits renal tubular transport

Levofloxacin

Of the FQ’s, has the HIGHEST renal elimination. Best for urinary penetration.
BEST for lung penetration. Think strep pneumo and respiratory infections.
Covers PSEUDOMONAS
Covers MSSA (not MRSA)

Moxifloxacin

Of the FQs, LOWEST renal elimination. Not useful for UTIs
Of the FQs, HIGHEST half-life
2nd best for lung penetration. Think strep pneumo and respiratory infections.
Covers ANAEROBES
Covers MRSA
Does NOT cover pseudomonas

Gemifloxacin

Low renal penetration. Not useful for UTIs.

Delafloxacin

Of the FQs, LOWEST oral bioavailability
Like Levo and Moxi, FDA approved for CAP
FDA approved for acute bacterial skin and skin structure infections
Covers ANAEROBES
Covers PSEUDOMONAS
Covers MRSA
The only FQ that covers E. Faecalis (not faecium)
Does NOT produce QT prolongation effects
Package label states that FQs should be used when there is no alternatives for all FQs EXCEPT Delafloxacin

Macrolides (Erythromycin, Clarithromycin, Azithromycin)

Erythromycin

WORST gram-negative activity (A>C>E)
Oral base formulation needs enteric coating. Esters are more resistant/better absorbed.
The BEST absorbed erythromycin ester oral formulation is erythromycin estolate.
Don’t take any erythromycin EXCEPT E. estolate with food (does not affect estolate version)
Absorbed in duodenum
Minimal distribution into CSF. Highly protein bound.
NO adjustment required in renal impairment (bile and fecal elimination)
Crosses placenta/into breast milk
Erythromycin is the ONLY approved macrolide for Diptheria infections
Unique off label use – Gastroparesis (prokinetic agent)
Of the macrolides, has the GREATEST chance of causing hepatotoxicity (starts 10-20 days after treatment [long term use])
Strongly inhibits CYP3A4

Clarithromycin

Has a methoxy instead of a hydroxy at C6
Clarithromycin as a parent drug is active, and it also has an active metabolite.
BEST gram-positive activity (C>E>A)
Resistance found in mycobacterium & H. pylori
The only macrolide (at least from lecture) NOT available IV
First pass reduces F to 50-55% (HIGHEST F)
May be given WITH or WITHOUT food
- Give ER versions with food, though.
Metabolized by the LIVER. Metabolism is SATURABLE.
- Higher doses equate to longer half-lives
20-40% excreted in urine. ADJUST dose if CrCl < 30mL/min
NO dosage adjustment w/ hepatic impairment
GI, cardiac, and hepatotoxic effects LESS than erythromycin
Use with H. Pylori infection
Use with Mycobacterial infections (M. leprae and M. Avium Intracellulare)
Use with Resp. tract infections
Like erythromycin, strong inhibitor of CYP3A4

Azithromycin

Instead of 14 membered rings, has 15 carbon ring.
Has a nitrogen in place of carbonyl group at 9a (in place of ketone found in erythromycin)
WORST gram-positive activity (C>E>A)
BEST gram-negative activity (A>C>E)
Absorbed rapidly but incompletely (F=30-40%)
Has high drug concentrations within cells
Excreted via biliary route
Very little (12%) excreted in the urine
Has the LONGEST half life (40-68h) due to its tissue binding ability
GI, cardiac, and hepatotoxic effects LESS than erythromycin
Of the Macrolides, Azithromycin is preferred in resp. tract infections
- Chlamydia, pertussis, mycobacterial infections
Z-pak dosing: 500mg PO day 1, then 250mg PO day 2-5
A single 1g dose can be given for uncomplicated gonococcal urethritis due to C. trachomatis.
LOWEST likelihood of the macrolides to cause drug interactions

Fosfomycin

Fosfomycin

F is low – use limited to UTIs (bladder infections; cystitis)
Enters the cell via two active transport mechanisms:
- Glycerophosphate transport (GLpT)
- Hexose phosphate uptake system (UhpT)
Blocks cell wall synthesis; bactericidal
Binds the MurA enzyme by acting as a phosphoenolpyruvate analog and blocks the initial step in peptidoglycan synthesis.
Oral ONLY
Short half-life, renal elimination
Active vs MSSA/MRSA/Enterococcus/UTI-related gram negatives, among others
NOT ACTIVE against S. Saprophyticus**, Stenotrophomonas, Burkholderia, anaerobes
Resistance
- MurA alterations
- Overexpression of enolpyruvyl transferase – overpowers Fosfomycin activity.
- Transport alterations (remember it has to get transported by GLpT & UhpT )
- Fos A, Fos B, Fos C (Fosfomycin modifying enzymes)
GI: Diarrhea/nausea most common
Interactions:
- Drugs that stimulate motility decrease absorption of Fosfomycin
- Fosfomycin might minimize aminoglycoside accumulation.. less nephrotoxicity?
Uses:
- Uncomplicated acute cystitis
- Complicated cystitis
- Prophylaxis
Given as one dose
It is expensive

Nitrofurantoin

Nitrofurantoin

Macrobid (macrocrystalline) is more tolerable than microcrystalline (less D/N)
Has short half-life and is eliminated in urine and bile
Alkaline urine may reduce its effectiveness
It relies on concentrating in the urine to work, so impaired renal function may have limited effectiveness
It does not penetrate well into kidneys, CSF, eyes etc. Only useful for bladder infections (cystitis)
Take with food!!
Technically contraindicated in CrCl <60ml/min but still used at 40+ mL/min
CONTRAINDICATED in pregnancy >38 weeks and neonates <1 month
ADEs
- GI: N/V (dose related)
- Pulmonary toxicity/fibrosis with long-term use
- Urine discoloration (brown)
- False positive glycosuria test
- Magnesium antacids (reduces nitro absorption)
- Probenecid (increases Nitro serum concentration)
Only for cystitis, typical treatment duration 5 days. Primarily GI sx.
Consider Fosfomycin for long-term use (prophylaxis)

Polymyxins (Colistin, Polymyxin B)

Colistin

IV or inhalation only (inhalation optimizes lung exposure)
Poor penetration to lung, tissue, pericardial fluid, CSF
Colistin is given as an INACTIVE PRODRUG (Colistimethate sodium, CMS)
- CMS gets cleared by renal elimination OR converted to Colistin (active)
Colistin is eliminated by non-renal clearance – the high concentrations found in urine are CMS being converted to colistin.
Because of being found in urine, it is BETTER than polymyxin B for UTIs
Colistin requires a loading dose to be used
- When calculating dose, CrCl is calculated with Jellife equation
- Actual or ideal BW is used, whichever is lower

Polymyxin B

IV only
NON-renal elimination
Unlike colistin, administered in ACTIVE form
Gets REABSORBED in kidney, resulting in low urinary concentrations; not useful for UTIs
Dosing must be adjusted for renal function
Of the two, considered more reliable due to being administered in active form

Lincosamides (Clindamycin)

Clindamycin

BacterioSTATIC (like macrolides)
Inhibits the 50S subunit (like macrolides)
- Inhibits peptide bond formation (inhibits translocation, like macrolides)
Spectrum is gram-positive and anaerobes
- Strep, MSSA/MRSA
- Anaerobes: bacteroides, prevotella, fusobacterium, Clostridium
  - C. perfringens only, NOT C. Difficile
- Pneomucystis jirovecii (fungus)
- Protozoa (Toxoplasma gondii and plasmodium falciparum)
Resistance to clindamycin (same as macrolides) – erm gene.. methylates adenine of 23s RNA of the 50s subunit. This can be constitutive or inducible.
- Thus, cross resistance to macrolides and clindamycin and streptogramin B
- Phenotypically, bacteria with this gene would be called “MLSB”
- Resistance is plasmid mediated.
The D test (for Staph – only staph have the erm gene. Strep have the mef gene)
- This test is useful when your staph isolate is erythromycin resistant and clindamycin susceptible.
  - If this occurs, you need to perform a D-test.
    - D-test result positive: Staph can become resistant to clindamycin during therapy. Do not use.
    - D-test negative: Can use clindamycin for therapy.
Oral form nearly COMPLETLEY absorbed (available PO/IV/IM, and topical)
Penetrates most fluid/tissues EXCEPT CSF
Clindamycin is metabolized by the liver and thus may ACCUMULATE in severe hepatic failure
After IV therapy stopped, antimicrobial activity can persist in feces for >5 days
NO ADJUSTMENT in renal failure or hepatic disease – monitor
Uses:
- SSTIs (INCLUDING CA-MRSA)
- Respiratory tract infections (due to its anaerobic activity)
  - Abscesses, anaerobic pleural space infections
- Other anaerobic infections
  - (infections of the female genital tract)
  - Prophylaxis of endocarditis in patients with valvular disease undergoing certain dental procedures (pts. With penicillin allergies)
- WITH primaquine, alternative agent for pneumocystis jirovecii pneumonia
- WITH Pyrimethamine, AIDS-related toxoplasmic encephalitis
- Surgical prophylaxis
- Topical form for acne vulgaris, bacterial vaginosis
ADEs
- GI: N/V/D; mostly with PO
- Big risk for C. Diff infection
- May block neuromuscular transmission
- Weigh benefit vs risk in pregnancy
- AVOID while breast feeding

Nitroimidazoles (Metronidazole)

Metronidazole

INERT (prodrug) until activated in the cell
MOA:
- 1) Drug ENTERS the cell via passive diffusion
- 2) An ELECTRON TRANSFER to metronidazole’s nitro group occurs.
  - Results in a reactive free radical
  - The free radical INTERACTS WITH DNA
- 3) DNA synthesis is INHIBITED and damaged. Oxidation, breaks. Etc.
- 4) DNA DEGRADES, host cell DIES. Then there is a RELEASE of INACTIVE END PRODUCTS of the drug.
ANAEROBES ONLY does not work in aerobes
- Mainly Bacteroides (low resistance)
- Can also be used for parasitic infections and H pylori
Oral caps/tabs, IV, topicals (creams/gels/lotions/vaginal gels)
NO dosage adjustment in renal impairment
50% dose reduction in severe hepatic impairment
100% F; IV to PO conversion 1:1
Protein binding <20%, low protein binding and very lipophilic.
Large Vd makes it effective for getting into tissues
- PREFERRED AGENT FOR CNS ANAEROBIC INFECTIONS
ADEs
- CNS (ataxia, encephalopathy, seizure, aseptic meningitis)
- Peripheral neuropathy (w/ prolonged use, reversible. Most common)
- Disulfiram-like reaction (Antabuse reaction)
SAFE pregnancy; defer breastfeeding if taking large doses of metronidazole
Bacteroides resistance: nim genes