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Title: shock

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shock

??Introduction
1. 1731. Le Dran French
He first used shock to describe
the severe condition of
the patient of hurt.

2. 1895 Warren
describe the clinical manifestations
of shock

the face is pale or cyanosis
cold and clammy skin
rapid and thready pulse
oliguria
apathy
?hypotension (Crile)

Mechanism
peripheral circulatory failure
Vascular center paralysis
Treatment pressor

1960s
The theory of microcirculation
Sympathetic-adrenal medulla hypersympathetic
70s Cellular metabolic disturbance
80s septic shock

??Concept
Causes disturbance blood flow of
microcirculation functional and
metabolic disorders of the vital organs
Inadequate tissue perfusion

??Etiology and classification of shock
? Etiology
1. Blood loss and body fluid loss
SIHR/SBP
SI Blood Loss
0.5 10 compensation
1.0 20 30 shock
1.5 50 death

fluid loss vomit. diarrhea
collapse
2.Burn/trauma pain, plasma loss burn
shock, infection shock(late)

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4. Infection infectious shock
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?endotoxicshockLPS,
pseudosympathetic
septic shock
hypodynamic shock low-output,cold shock
hyperdynamicshockhigh-output,warm shock
(pink,dry), NO,PGI,PGE

5. Anaphylaxis anaphylaxic shock
6. Cardiogenic shock
7. Neurogenic shock
? classification of shock
2. 1. According to the cause of shock

According to the start problem
1) Hypovolemic shock
CVP,CO,artery blood pressure PR
2) Vasogenic shock 1/5 cap opening
Cardiogenic shock CO CIlt2.2L/min.m2
myoardiumgenic shock
non myoardiumgenic shock

?? Periods and pathogenesis
? early phase of shock (ischemic phase,
compensatory stage, ?phase)

1.changes of the microcirculation and its
mechanism
1)Microcirculation

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contraction
micro-artery
Metarteriole
precapillary sphincter
Micro-vein

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?Axial flow particles flow
? a. Capillaries were closed,
b.thoroughfare channel and Arteriovenous
shunts are open
ß-receptor
? perfusion flow perfusion lt flow

2) mechanism
Sympathetic-adrenal-medullary system
Renin-angiotensin system

(1)BP sympathetic contraction of
the
pain nerve
artery and vein
Endotoxin
(2)sympathetic renal blood flow
angiotesin
nervous system catecholamine

(3) endothelin (ET)
tissue impairment
(4)TXA2
lecithoid (??)

Opposite effectTNF,NO,lactic acid
3) compensatory meaning
Bp self-transfusion
self-blood transfusion
CO
HR
redistribution of blood flow

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2. Manifestations

? mental status dysphoria, anxiety,
consciousness
?skin cold and clammy, paleness of
complexion
?cardiovascular system
rapid and thready pulse,
BP,
pulse pressure
?urine oliguria

? shock phase (stage of stagnant anoxia, ? phase)

1. changes of microcirculation and its mechanism
1)Microcirculation
Dilation
micro-artery.
Metarteriole.
precapillary sphincter
perfusion flow perfusion gt flow

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Hemorheology
RBC acetylneuraminate(???) COOH
bring negative charge
sulfate(endothelium) negative charge
stack(??), sludge

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2) mechanism
Hypoxia
Histamine vasodilation congestion
post-capillary resistance gt pre-capillary
resistance
Kinin(??) permeability blood
Histamine of capillaries volume
hypoxia of brain and heart

LPS,TNF,IL-1
P-selectin\E- selectin
ICAM-1,VCAM( endothelium )
WBC adhesion to endothelium cell

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perfusion flow perfusion gt flow
3)effects on body
a. Bp
b. Peripherial resistance coronary artery

2. manifestations
?mental status faint coma
?skin cyanosis ,veined marble
?BP heart sound slight pulse(septic
shock full pulse)
?urine oliguria or anuria

? Terminal shock (phase of DIC, ? stage,
refractory shock stage,irreversible stage,)
microcirculatory failure stage)
VSMC in wall of vessel of micromirculation(
paralysis)

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1.Formation of DIC
1)concentration fibrinogen
of blood velocity of blood flow
2) acidosis damage of intrinsic blood
endotoxin endothelium coagulation

3)traumatic factor ? extrinsic
blood
shock (TF)
coagulation
Common pathway ?

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intrinsic blood coagulation
extrinsic blood coagulation
Cascade trigger Dominoes push over
coagulation
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4)progressive decrease of vessel reaction
Vessel to CA
H , NO VSMC KATP open Kout
Ca2in
PGI

2.changes of microcirculation
no perfusion , no flow , no-reflow(, WBC
sequestration
3.Effects on body
a.venous return to heart
b.Coagulation bleeding
c. Thrombosis and embolism

4. Manifestations
Cogulation bleeding

??Cellular metabolism alteration
(?) Dysfunction of Cellular metabolism
a. hypoxia glycolysis
lactic acidosis
b. ATP Na-K pump cellular edema
c. metabolic acidosis

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Cells damage

mitochondria
hypaoxia acidosis
free radical
lysosome
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Experiment
The function of WBC leucocyte deficiency
Copy shock model of Rat
Test group 40mmHg all alive
Control 36 death
Test group 30mmHg all alive
Control 100 death

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(?)Injury and apoptosis of cells 2002
WHO You ,he or she
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apoptosis of cells gene regulation
procedure death
Physiologic
pathologic

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.
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Activating Endonuclease degrade DNA
180-200bp oligonucleotide
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(?)inflammatory mediator
TNF \ IL-1,2,6,8 \ TXA2
Anti- inflammatory mediator
IL-4, 10\ NO\ PGI2
(?)signal transduction
1.NF-?B
2.MAPK

?systemic inflammatory response syndrome(SIRS)
1.Introduction inflammatory medium release
body reaction
38? lt T lt36?
HRgt 90?/min
Rgt 20?/min or PaCO2 lt4.0kPa
4109/L gt WBC gt12109/L
two points of above SIRS

2. Etiology and classification
Etiology
a.an-infective agent trauma,operation
ischemia-reperfusion
b. Infective agent microorganism 70
second hit

3.period of SIRS
1) Inflammatory cells activity
2) Inflammatory mediator spillover
local whole body,
3) SIRS/CARS imbalance
inflammatory mediator overflow
mixed antagonist
compensatory anti- inflammation response
syndrom(CARS)
response syndrom(CARS)

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Pathogenesis
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multiple organ dysfunction
symdromeMODS

Multiple organ dysfunction syndrome
1975? multiple organ failure(MOF)
1991? multiple organ dysfunction
symdrome(MODS)

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?????? Sequential system failure Tilney 1973
?????????????? Multiple progressive or sequential systems failure Baue 1975
??????? multiple organ failure Eiseman 1977
?????? remote organ failure Polk 1977
??????? multiple systems organ failure Fry 1980
???????? acute organ-system failure Knaus 1985
?????????? multiple organ dysfunction syndrome ACCP/SCCM 1991
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1. Concept of MODS
Organ function in normal ,shock ,large operation
dysfunction /failure of two or more than
two organs occur at the same time or one after
another (36hs) .

2. classification
a. rapid single-phase 12-36h
Causes dysfunction of two organs
b. delayed two-phase after 1-3week
inflammative factor second hit

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3.important organ failure

1)Acute renal failure(shock kidney)
early stage renal blood flow
functional renal failure GFR
oliguria
late stage acute tubular necrosis(ATN
)
parenchymal renal
failure
(?????)

Grade of renal failure
Endogenous creatinine clearance rate
Pcr(plasma creatinine)
? Pcr gt1.8mg/dl
? Pcr gt2.5mg/dl
? Pcr gt5.0mg/dl, hemodialysis(????)

2)Acute respiratory failure(shock lung)
congestion
edema
thrombosis
atelectasis
formation of hyaline membrane
lung bleeding

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Korea,Vietnam?? war hemodialysis
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Grade of respiratory dysfunction
? PaCO2 lt 33mmHg, PaO2 gt 60mmHg
? PaO2 lt 60mmHg ,cyanosis
? O2 50 ,breathing apparatus assist,
PaO2 lt 50mmHg , PaCO2

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3)Cardiac functional diaturbance(shock
heart)

early stage compensation
late stage
coronary blood flow
acidosis?ATP
hyperkalemia heart
failure
MDF
DIC of myocardium

Grade of cardial dysfunction
CI(cardiac index) 3.0-3.5L/min/ m2
?CIlt3.0 L/min/ m2
?CIlt2.0 L/min/ m2
?CIlt1.5L/min/ m2 , drugs

4) Brain function disturbance(shock brain)
early stage consciousness
late stage ischemia hypoxia
brain edema faint?coma

5) Hepatic dysfunction
a.Kupffers cell IL-8 PMN
sequestration
b.xanthine oxidase release O2 -
c.liver function acidosis,endotoxemia
icterus

Grade of liver dysfunction
Bilirubin
?gt 2.0 mg/dl icterus
? gt 4.0 mg/dl
? gt 8.0 mg/dl

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6) Digestive tract
stomach ischemia, DIC, congestion
stress ulcer
intestine perfusion barrier
function
microthrombus
bacteria\toxin get
into blood

?? Principle of treatment
1. Restore blood volume
Volume of transfuse 5 times lose
CVP (right heart)
PAWP (left heart)
2. Treatment of acidosis

What will be transfused?
Blood
crystalloid 0.9NaCl (sodium chloride)Saline,isot
onic solution)
water 10 glucose glycogen
colloid plasma ,to keep osmotic pressure

3. Application of vasoactive drugs
pressors drugs mortality
vasodilation drugs?(blood volume,CVP,Bp)
From Lab to bedside, from bedside to Lab
4. Protection of cells hormone
5. Antagonists of humoral factor
Benzantin histamine
SOD O2 -

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Case 1

A 62-year-old man was brought to the emergency
room by his son,who reported that the
man(documented diabetes) had been eating poorly
for 2 days and difficult to arouse that morning.
On exam
The patient would open his eyes and mumble
incoherently in response to pain.T38.6?
BP75/40mmHg, HR 124/min,his skin was warm.
Lab data
WBC 19.5103/mm3,oliguria, cloudy urine. Blood
was sent for culture.

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Treatment

Volume
Antibiotics
Pressors PRN

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Case 2

A 67-year-old-femal arrived in the emergency room
complaining of chest pain and severe weakness
present for 12 hours.These symptoms had been
preceded by several days of poor appetite,
nausea( ??)and vomiting.
On exam
P 110/min,Bp85/50mmHg.ECG suggesting an evolving
inferior myocardial infarction

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Treatment