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Samenvatting INFECTIEZIEKTEN-DEEL FARMACOKINETIEK

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Ander belangrijk onderdeel van het examen gegeven door Prof Claus. Dit moeilijk stuk wordt duidelijk uitgelegd en samengevat in dit document. Ook op dit onderdeel moet je afzonderlijk geslaagd zijn om te kunnen slagen voor het vak. Ik behaalde 1ste zit door dit document. Het bevat de inhoud van de slides + wat er gezegd is geweest in de les

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DEEL II: FARMACOKINETIEK
EN FARMACODYNAMIEK

,INHOUDSOPGAVE

1. ANTIBACTERIËLE MIDDELEN...................................................................................................... 4
a. 𝛽-lactam antibiotica ................................................................................................................. 4
B. macroliden ................................................................................................................................. 4
C. tetracyclines............................................................................................................................... 5

D. clindamycine en lincomycine ...................................................................................................... 5
E. chinolonen (= fluoroquinolones) ................................................................................................... 5
F. sulfonamiden .............................................................................................................................. 6
G. urinaire antibacteriele middelen .................................................................................................. 6
H. tuberculostatica ......................................................................................................................... 6
I. aminoglycosiden .......................................................................................................................... 6
J. glycopeptiden ............................................................................................................................... 7
K. diverse antibiotica ....................................................................................................................... 7

1. definitie ................................................................................................................................ 8

2. PARAMETERS ........................................................................................................................ 8
max concentratie ............................................................................................................................. 8
Halfwaarde tijd ................................................................................................................................ 9

Oppervlakte onder de curve ............................................................................................................. 9
plasma-Proteïne binding .................................................................................................................. 9

Biologische beschikbaarheid (BB)..................................................................................................... 9

3. ADME .................................................................................................................................. 10

A. absorptie ................................................................................................................................10
B. Distributie ...............................................................................................................................11
C. Eliminatie ...............................................................................................................................12

1. Definitie............................................................................................................................... 13

2. Dosis respons curve ............................................................................................................. 13

3. Curve die ons iets zegt over PK en PD .................................................................................... 13

1. van mic naar geschikte ab keuze ........................................................................................... 14
A. gevoeligheidsbepalingen .........................................................................................................14
B. Raportering van de gevoeligheidsbepaling door het klinisch labo ...............................................17

2. begrip breekpunt.................................................................................................................. 18
A. definities ................................................................................................................................18



2

, B. eucast ....................................................................................................................................18
C. Vuistregels bij de interpretatie van een antibiogram ..................................................................20
D. ambulante praktijk ..................................................................................................................22

3. Groepen van antibiotica ingedeeld volgens PK-PD kenmerken ............................................... 22
algemeen .......................................................................................................................................22
A. tijdsafhankelijke AB .................................................................................................................24
B. AUC over MIC met een tijdsafhankelijke factor..........................................................................26
C. concentratie afhankelijke AB (Cmax/MIC) ................................................................................30
D. Tijdsafhankelijk VS concentratie afhankelijk .............................................................................31

4. therapie duur ....................................................................................................................... 32
therapieduur vs posologie ...............................................................................................................32
vroeger vs nu ..................................................................................................................................32

5. casussen ............................................................................................................................. 32

1. intensieve zorg patiënten ..................................................................................................... 33
A. instellen van antibiotherapie ....................................................................................................33

B. wijzigingen in PK/PD ................................................................................................................34
C. Optimaal dosseren bij IZ ..........................................................................................................37

2. Kinderen .............................................................................................................................. 39
A. Achtergrond ............................................................................................................................39

B. Farmacokinetiek bij kinderen ...................................................................................................40
C. oplossen van casussen ...........................................................................................................42

3. Ouderen .............................................................................................................................. 44
A. farmacokinetiek ......................................................................................................................44
B. casussen ................................................................................................................................46

4. CYSTIC FIBROSIS PATIËNTEN ............................................................................................... 47

Achtergrond ...................................................................................................................................47
Behandeling ...................................................................................................................................48

5. Obese patiënten...................................................................................................................... 52

Achtergrond ...................................................................................................................................52
Invloed op farmacokinetiek .............................................................................................................52

Kwantificatie van obesitas ...............................................................................................................53




3

, H1: KLASSEN VAN ANTIBIOTICA
1. ANTIBACTERIËLE MIDDELEN

A. 𝛽-LACTAM ANTIBIOTICA


PENICILLINES

• Benzylpenicilline
• Feneticilline
• Flucloxacilline
• Amoxicilline
• Carboxypenicillines
• Acylureïdopenicillines


CEFALOSPORINES

• Cefadroxil
• Cefalexine
• Cefazoline
• Cefuroxim
• Cefotaxim
• Ceftazidim
• Ceftriaxon
• Cefepim
• Ceftaroline
• Ceftolozaan


CARBAPENEMS

• Meropenem


MONOBACTAMS

• Azactam
• Cayston

B. MACROLIDEN


ERYTHROMYCINE




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