Role of Pharmacist Flashcards

1
Q

Read bit in lecture on guidelines

A

Read bit in lecture on guidelines

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2
Q

Clostridium difficile characteristics Prevalence

A

Gram +ve spore formning rods Present in the gut of up to 3% of healthy adults Inhibited by normal gut flora

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3
Q

C. diff cycle

A
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4
Q

Risk factors C. diff infection

A

Elderly Recent antibiotic use, (1/12) (NG-tubes, PPIs)

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5
Q

Symptoms of C. diff infection

A

Diarrhoea (BSC 6-7) Often with mucus Offensive smell

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6
Q

Secondary symptoms of C.diff

A

raised CRP/WCC

Pyrexia

Toxic confusional state in elderly

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7
Q

C. diff disease outcomes

A
  • Mild disease; self-limiting.
  • Severe disease; Pseudomembraneous Colitis. Damaged mucosa Pseudomembranes
  • Clinical signs (PMC): - Abdominal distension, High WCC, usually diarrhoea
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8
Q

C. diff management

A
  • Stool sample for toxin.
  • Patient isolation, strict enteric precautions, perfect hand hygiene (soap and water).
  • Stool chart and daily monitoring of stools
  • Stop offending antibiotics.
  • Review drugs that may cause diarrhoea (PPIs, Laxatives etc.)
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9
Q

Current standard C. diff treatment

A

PO Vancomycin

  • Main C.diff treatment - Oral not IV 125-250mg four times a day Better efficacy in severely ill
  • Higher dose 250-500mg with adjunct IV metronidazole (?ileus) if complicated – fulminant disease.

PO Fidaxomicin

Lower relapse rate vs Vanc. (12-15% vs 25-27%)

  • Consider for: - Severe disease in patients with concurrent abx. and co-morbidities - Recurrence if C.diff within ~30 days £1350/course
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10
Q

Emerging C. diff therapies

A
  • Rifaximin IV
  • Immunoglobulins, Bezlotoxumab
  • Faecal Microbiota Transplants
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11
Q

uses of FMT

A

Appears to be highly effective for the treatment of CDI: 90% resolution across 33 case series

Indication:

  • Recurrent CDI
  • Refractory CDI
  • Acute Severe CDI: not initial therapy
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12
Q

Antibiots associated with C.diff

A
  • 10-40% of patients exposed to antibiotics.
  • Most/all antibiotics can cause Antibiotic associated diarrhoea (AAD) and C.diff. 25% of AAD.
  • High-Risk – mostly “broad- spectrum” -
  • Clindamycin
  • Cephalosporins
  • penicillins (e.g. co-amoxiclav piperacillin/tazobactam) -
  • Quinolones (e.g. ciprofloxacin)
  • Carbapenems
  • Erythromycin also causes diarrhoea by stimulating motility.
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13
Q

Examples of lower risk (narrow spectrum) antibiotics

A
  • Tetracyclines (e.g. doxycycline)
  • Metronidazole
  • Glycopeptides (e.g. vancomycin) – limited GI exposure
  • Aminoglycosides (e.g. gentamicin) – limited GI exposure
  • Flucloxacillin, penicillin V, benzylpenicillin Trimethoprim
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14
Q

When to use Therapeutic drug monitoring?

A

Drug with narrow therapeutic index E.G Aminoglycosides (Gentamicin)

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15
Q

When to use aminoglycosides and considerations

A
  • Effective against most Gram –ve bacteria (inc Pseudomonas sp.) and Staph. aureus (inc. MRSA).
  • Sufficient peak for efficacy. Low trough before re-dosing to reduce Nephrotoxicity/ toxicity.
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16
Q

Adult gentamicin dosing

A
  • Once daily gentamicin = 4-7mg/kg/day
  • Multiple daily dosing = 3-5mg/kg in divided doses
  • Dose altered in renal impairment.
17
Q

Monitoring gentamicin

A

Multiple daily dosing = Peaks and Trough taken around 3rd or 4th dose

Once daily gentamicin = Trough levels only, prior to second dose.

Target range: - Once daily gentamicin:

  • Trough = <1mg/L,
  • Peak = not measured

Multiple daily dosing:

  • Trough = <2mg/L
  • Peak = Usually 5-10mg/L

Pseudomonas sp. 7-10mg/L . For synergy in streptococcal or enterococcal infections (e.g. endocarditis) 3-5mg/L

18
Q

Considerations for gentamicin

A

Gentamicin major cause of preventable drug related toxicity (nephro- and ototoxicity).

  • Risk increased by other nephrotoxic drugs (e.g. NSAIDs, Vancomycin)
  • Monitor renal function Routinely: Twice weekly levels
  • Decline in renal function/urine output. - Once daily - immediate trough level and await result before re-dosing.
  • Multiple daily dosing – levels around next dose.
19
Q
A