GENERAL ANAESTHESIA Jozef Firment, MD PhD Department of Anaesthesiology & Intensive Care Medicine Šafárik University Faculty of Medicine, Košice A I S E H DEFINITION T S E A N A • (an) aisthetos = (un) perception L A R E N • general anaesthesia = „narcose“ E G • regional anaesthesia = local tn e m r iF 2 A I S SURGICAL STRESS MAP E H T Barash, 1997 S E Theoretical Plasma Drug A Concentration for Adequate N A Anaesthesia L A Intubation R E N E Incision G n o Mount r i o t a Lake Surgery e r Recovery s t n Prep. n e Plains o c p n Anxiety s Peritoneal Bowel/ o e c R Mound Traction Vascular ICU a s m s Clamping Highlands Sleep River e s r a tn t l e S P m r iF Duration of Surgery 3 A I S E PHARMACO-ANAESTHESIA H T S METHODS E A N A L • Inhalational anaesthesia ... VIMA A R E • Intravenous anaesthesia... TIVA N E G • Intramuscular • Rectal • Combined anaesthesia tn e m r iF 4 A I BASAL PARTS OF GA S E H T S E BIS Monitoring A N Consciousness/Hypnosis A L A R E N E G Balanced Anaesthesia Muscle Analgesia relaxation/ Areflexia Hemodynamic Peripheral tn Monitoring Nerve Stimulator e m r iF Monitoring Monitoring Anaesthetic Endpoints 5 A CIRCULATORY EFFECTS I S E H INHAL. ANAESTHETICS T S E (Barash, 1997) A N A •  BP according to dose (vasodiltion,  C.O., L cardiodepresion,  sympat. activity) A R •  consumption O about 10-15% E 2 N •  blood flow in liver, kidneys and gut, E G  in brain, muscles & skin • N O SVR, PVR and BP,  C.O. 2 • Sensibilisation myokardium to catecholamins:  in children, HAL > ENF > ISO > DES > SEV (more in CO , more with thiopental) 2 • No influence to pacemaker functions tn e m • No coronary steal efect in man r iF 6 A RESPIRATORY EFFECTS I S E H INHAL. ANAESTHETICS T S E (Barash, 1997) A N A • All  V and bronchodilational effect L T A • Bloc histamin effects on bronchi – bronch. R E N asthma treatment: HAL, SEV E G • Respiratory depresion : N O>HAL>ISO>DES 2 • No influence to hypoxic pulmonary hypertension • Up to 3x increase effects of musclerelaxants tn e m r iF 7 A CNS EFFECTS OF I S E H INHAL. ANAESTHETICS T S E (Barash, 1997) A N •  intelectual functions, HAL for 2-8 days (B?) A L A •  intensity of cerebral metabolism (CMRO ): R 2 E ISO > EFL>HAL. N E • Vasodilat. cerebr. a. &  pressure CSF: G HAL>ISO=DES=SEV, • HAL > ISO influence production & absorbtion CSF • Light hypocapnia - lower ICP in ISO than HAL • Autoregulation to CO is more blocked by HAL than 2 ISO tn e m • Epi EFL r iF 8 A I S E TOXICITY H T S E A • HAL = hepatotoxicity (imuno, repeated N A expositions) L A • N O = hematotoxicity „perniciose“ R 2 E N anaemia E G • In septic pat. weakening Ne and Le functions • Change platelets functions • Myometrium relaxation – bleeding during C.s. (HAL > 0,5, ISO > 1,0) tn e m Barash, 1997 r iF 9 A I DISTRIBUTION COEFF. S E H ANAESTHETICS (BLOOD / GAS) T S E A ) N s a A g : L Less solubility = faster onset d 3 A o R o 2.5 l b E ( N tn 1.8 2 e E i c G i 1.43 f f e o c 1 0.65 n o 0.45 0.47 i t u b i r t s i Desflurane Nitrous Sevoflurane Isoflurane Enflurane Halothane D Oxide tn e m r iF Miller. Anesthesia. 4th ed. Churchill Livingston, 1994; Data on file, Abbott Laboratories Inc. 10