Zusammenfassung
Die beatmungsassoziierte Pneumonie ist die bedeutendste nosokomiale Infektion in der
Intensivmedizin. Eine frühzeitige adäquate Antibiotikatherapie hat höchste Priorität
für das Outcome der Patienten; die Frage nach der optimalen diagnostischen Strategie
steht dahinter zurück. Die initiale Antibiotikawahl richtet sich danach, ob multiresistente
Erreger zu erwarten sind. Im Risikofall ist eine empirische Kombinationsbehandlung
indiziert, die vorangegangene Antibiotikabehandlungen und lokale Resistenzmuster berücksichtigt.
Die Reevaluation und Deeskalation der Therapie anhand der mikrobiologischen Befunde
und die Begrenzung der Therapiedauer auf eine Woche sind entscheidend, um den Einsatz
von Breit-spektrum-Antibiotika und die Selektion multiresistenter Erreger einzudämmen.
Summary
Ventilator-associated pneumonia remains the most serious nosocomial infection in critically
ill patients. Providing appropriate antibiotic therapy promptly is crucial for successful
treatment; whereas the diagnostic approach seems to play a minor role. The empirical
antibiotic therapy should be guided by the risk for infections due to multiresistant
bacteria. For patients at risk a combination therapy, considering local resistance
data and formerly applied antibiotic substances, is recommended. Reevaluation and
deescalation of antibiotic therapy based on microbiological culture results and discontinuation
of antimicrobial treatment after one week is essential for the control of broadspectrum
antibiotic use and antibiotic resistance.
Schlüsselwörter:
beatmungsassoziierte Pneumonie - multiresistente Erreger - Pseudomonas aeruginosa
- methicillinresistenter Staphylococcus aureus (MRSA) - Acinetobacter ssp
Key words:
ventilator-associated pneumonia - multiresistant microorganisms - Pseudomonas aeruginosa
- methicillin-resistant Staphylococcus aureus (MRSA) - Acinetobacter ssp
Kernaussagen
-
Beatmete Patienten haben ein erheblich höheres Pneumonierisiko als spontan atmende
Patienten; das Risiko steigt kumulativ mit der Beatmungsdauer.
-
Das Auftreten einer beatmungsassoziierten Pneumonie wird in erster Linie durch die
Intubation begünstigt; entsprechend kann die Pneumoniehäufigkeit durch noninvasive
Beatmung gesenkt werden.
-
Weitere sinnvolle Maßnahmen der Pneumonieprävention sind oropharyngeale Dekontamination,
Oberkörperhochlagerung und subglottische Sekretabsaugung. Sedativa sollten restriktiv
eingesetzt werden, um die Beatmungszeiten und das damit assoziierte Pneumonierisiko
möglichst gering zu halten.
-
Ein allgemein anerkannter Goldstandard für die Diagnostik der VAP existiert nicht.
Anhand klinischer und radiologischer Zeichen kann die Diagnose nicht eindeutig gestellt
werden.
-
Durch bronchoskopische Gewinnung von Bronchialsekret in Kombination mit einer quantitativen
mikrobiologischen Untersuchung kann die Diagnose mit hoher Spezifität gestellt werden;
die Sensitivität ist allerdings - besonders bei bereits vorangegangener Antibiotikagabe
- weit unter 100 %. Wichtig für den Erregernachweis ist, dass Blutkulturen und Proben
von respiratorischen Sekreten vor Beginn der Antibiotikabehandlung gewonnen werden.
-
Die mikroskopische Untersuchung von Trachealsekret oder BAL kann Anhaltspunkte für
die Wahl der empirischen Antibiotikatherapie geben.
-
Die häufigsten Erreger der VAP sind Pseudomonas aeruginosa, Staphylococcus aureus
und Enterobacteriaceae. Wie weit mit multiresistenten Stämmen zu rechnen ist, hängt
ab von der Dauer des Krankenhausaufenthalts, vorangegangenen Antibiotikabehandlungen
sowie sog. Healthcare assoziierten Faktoren, wie z.B. Dialyse. Eine weitere wichtige
Rolle spielt die lokale Prävalenz multiresistenter Isolate in der jeweiligen Intensivstation.
-
Das Outcome der Patienten hängt von einer frühen und gleichzeitig adäquaten empirischen
Antibiotikabehandlung ab.
-
Um für einen möglichst hohen Anteil der Patienten noch vor Erhalt der mikrobiologischen
Befunde eine wirksame Therapie sicherzustellen, sollte in Fällen, die resistente Erreger
erwarten lassen, empirisch mit einer Kombination von zwei pseudomonaswirksamen Substanzen
sowie einem MRSA-wirksamen Präparat begonnen werden.
-
Nach Erhalt der mikrobiologischen Befunde sollte eine Reevaluation erfolgen, um die
Behandlung entweder anhand des Antibiogramms nachgewiesener Erreger auf Antibiotika
mit schmalerem Spektrum zu deeskalieren oder - falls sich der Verdacht auf eine Pneumonie
nicht bestätigen lässt - die Therapie zu beenden.
-
Bei gesicherter Pneumonie kann die Dauer der Antibiotikabehandlung auf acht Tage mit
einer einzelnen Substanz begrenzt werden; bei Pneumonien mit Pseudomonas aeruginosa
ist dieses Vorgehen allerdings umstritten.
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Dr. med. Alexandra Heininger
Prof. Dr. med. Klaus Unertl
Email: alexandra.heininger@med.uni-tuebingen.de
Email: klaus.unertl@med.uni-tuebingen.de