2. Contents:
Basic concepts
Normal Acid-Base homeostasis
Diagnosis of Acid-Base disorders
Types of acid-base disorders
Approach to acid-base disorders
3. Basic concepts:
pH: Signifies free H+ ion concentration
pH = – log [H+]
H+ plasma concentration (10- 1 to 10- 14 )
Acid: A substance that can “donate” H+ ion or when added to solution raises H+ ion (lowers pH).
Base: A substance that can “accept” H+ ion or when added to solution lowers H+ ion (raises pH).
Anion: An ion with negative charge (HCO3
- & Cl- )
Cation: An ion with positive charge (Na+, K+, Mg+)
Acidosis: Abnormal process or disease, which reduces pH due to increase in acid or decrease in
alkali.
Alkalosis: Abnormal process or disease, which increases pH due to decrease in acid or increase
in alkali.
Compensation: The body response to acid-base imbalance
Buffer: The chemical system that take up H+ or release H+ as conditions change
Volatile acids: Acids which can be excreted from body as gases by the lungs (breathed off)
Fixed acids (non-volatile): Acids which must be excreted in the urine (Not by breathed off)
Anion gap: The charge difference between unmeasured anions and cations
Unmeasured anions: Anionic proteins (albumin), Phosphate, sulphate & organic anions
Unmeasured cations: (Ca+2, Mg+2, K+)
(AG) = Na+ – (Cl- + HCO3
-) = 12±2 mEq/L (Normalvalue)
4. Normal acid-base homeostasis:
Homeostasis of pH is tightly controlled
Extracellular fluid pH = 7.4
Blood pH = 7.35 – 7.45
pH< 7.35: Acidosis (Acidemia)
pH> 7.45: Alkalosis (Alkalemia)
pH< 6.8 or > 8.0: death occurs
Normal range of Paco2 = 35-45 mmHg
Normal range of HCO3
- = 22-26 mEq/L
Respiratory compensation range (PaCO2= (1.5 × [HCO3
-]) + 8 ± 2)
Three lines of defense to regulate the body’s acid-base balance
Blood buffers (Bicarbonate – carbonic acid systems, Plasma proteins, Hemoglobin, Phosphates)
o Act fastest but have least buffering power
Respiratory mechanism (by excreting volatile acids, lung regulates Paco2 ) 50-75% efficacy rate
o Acts rapidly (seconds to minutes) & has double buffering power
Renal mechanism (the role is to maintain plasma HCO3
- concentration) 100% efficacy rate
o Starts within hours and takes 5-6 days for the peak effect & is the most powerful buffering
5. Types of acid-base disorder:
Simple acid-base disorders
Metabolic acidosis
o High-AG
o Non-AG (Hyperchloremic)
Metabolic alkalosis
Respiratory acidosis
o Acute
o Chronic
Respiratory alkalosis
o Acute
o Chronic
Mixed acid-base disorders
Metabolic acidosis + Respiratory acidosis or alkalosis
Metabolic alkalosis + Respiratory acidosis or alkalosis
Respiratory acidosis + Metabolic acidosis or alkalosis
Respiratory alkalosis + Metabolic acidosis or alkalosis
Metabolic acidosis + Metabolic alkalosis
Metabolic acidosis + Metabolic acidosis
6. Steps of acid-base diagnosis
Step 1: Determine the primary (main) disorder whether, it is metabolic or respiratory from blood pH,
HCO3
- and Paco2 values
Step 2: Determine the presence of mixed acid-base disorders by calculating the range of
compensatory responses
Step 3: Calculate the anion gap (AG)
Step 4: Calculate the corrected HCO3
- concentration, if the AG is increased
Step 5: Examine the patient to determine whether the clinical signs are compatible with the acid-base
analysis
8. Metabolic acidosis
• pH (Low)
• HCO3
- (Low)
• Paco2 (Low)
Causes:
High-AG (Increased unmeasured anions rather decrease unmeasured cations)
• Lactic acidosis
• Ketoacidosis
o Diabetic
o Alcoholic
o Starvation (Low carbohydrate diet)
• Toxins
• Renal failure (Renal acids and Albumin retention & increased anionic charge of albumin)
Non-AG
• GIS HCO3
- loss (Diarrhea, drugs such us CaCl2, Mg2so4 & Cholestramine)
• Renal acidosis (Hyperkalemia, Hypokalemia & Normokalemia)
• Others
Low-AG:
Increased unmeasured cations
Add external cations (Lithium intoxication)
Reduced plasma albumin (Nephrotic syndrome) & decrease anionic charge of albumin
Hyper viscosity and severe hyperlipidemia
Clinic:
CNS: Headache, Lethargy, Stupor, Coma
CVS: Cardiac function due to catecholamine release may be normal
Pulmonary edema
Hyperventilation (Kussmaul respiration)
Glucose intolerance
9. Medical treatment:
o The alkali therapy should be reserved for severe acidemia (pH<7.10)
o The pH should be slowly increased
o Except when the pt has no potential HCO3
- in plasma
o In the first determine delta-AG (pt AG – 10)
o Delta-AG determines wethere the anion acids are:
• Metabolizable (β-hydroxybutyrate, acetoacetate, lactate)
• Non-metabolizable ( CRF, Toxins ingestion)
o The pH should not to be increased to normal (Keep pH = 7.2)
o The K+ level must to be monitored during treatment (Risk of Hypokalemia)
o P/O (NaHCO3 or Shohls solution)
o IV (NaHCO3 50-100 meq 30-45 mins)
10. Lactic acidosis:
L-Lactate:
Type A: Poor tissue perfusion
Circulatory insufficiency (shock & HF)
Severe anemia
Mitochondrial enzyme defects & inhibitors (CO & Cyanide)
Type B: Aerobic disorders
Malignancies
HIV
DM
Renal or hepatic failure
Thiamine deficiency
Severe infections (Cholera & Malaria)
Seizures
Drugs/Toxins
Unknown bowel ischemia/infarction in pts with Cardiac decompensation receiving vasopressors (most common)
Pyro glutamic acidemia (Depletion of glutathione)
D-Lactate (formed by gut bacteria):
Jejunoileal bypass
Short bowel syndrome
Intestinal obstruction
11. Treatment of L-Lactate acidosis:
Correct underlying conditions
Restore tissue perfusion
Avoid vasopressors
Alkali therapy reserved for acute severe acidemia (pH<7.15)
HCO3
- disturbs cardiac function & enhance lactate production paradoxically
Because (HCO3
- stimulates phosphofructokinase)
The use of alkali in moderate acidemia is controversial
Infuse adequate NaHCO3 over 30-40 mins
NaHCO3 causes volume overload & HTN
After underlying conditions relapsed, lactate will be converted to HCO3
- & leads to alkali overshoot
12. Diabetic ketoacidosis (DKA):
Increased fatty acids metabolism
Accumulation of ketoacids (acetoacetate & β-hydroxybutyrate)
Often in IDDM
insulin cessation
Intercurrent illness which acutely increase insulin requirements (Infection, AGE,
Pancreatitis, MI)
Elevated-AG
Glucose> 300mg/dL
Volume depletion
HCO3
- therapy reserved for severe academia (pH< 7.1)
Insulin prevents production of ketones
Fluid restoration (N/S)
Hyperchloremic acidosis is common during fluid administration
IV insulin regular
13. Alcoholic ketoacidosis (AKA):
Abrupt alcohol cessation
Poor nutrition
Binge drinking, vomiting, abdominal pain, starvation & volume depletion
Ketones are elevated (β-hydroxybutyrate)
The mixed acid-base disorders are common
After volume correction (β-hydroxybutyrate shifts to acetoacetate) Ketosis & Ketonuria occurs
Normal renal function
Normal AG
Treatment:
IV (N/S & D5%)
Correct hypophosphatemia (12-24 hrs. after add), hypokalemia & hypomagnesaemia if existed
Hypophosphatemia exacerbated by D5% & if became severe leads to Rhambdomyolysis & Respiratory
arrest
Upper GIB, Pancreatitis & pneumonia also may accompany
14. Renal failure:
Hyperchloremic acidosis converted in high-AG acidosis
Pathogenesis made by poor filtration and reabsorption of organic anions
Disturbed net acids production by renal disease progression
Uremic acidosis made by reduced rate of ammonium production & excretion
In CKD, Retained acids buffered by bone alkaline salts (calcium carbonate)
Serum bicarbonate not decreased despite significant acids retention
Buffers participated out side the ECC (Extracellular compartment)
Significant bone mass loss
Increased urinary calcium excretion
Treatment:
Administrate Oral alkali 1-1.5 mmol/kg to maintain HCO3
- >22mmol/L
Shohl’s solution (sodium citrate) is equally effective NaHCO3
Citrate must never be given by aluminum-containing antacids (aluminum intoxication)
15. Non-AG Metabolic acidosis:
Alkali loss (Diarrhea & RTA)
Reciprocal changes in Cl- & HCO3
-
The absence of reciprocal changes suggest mix disorders
The acidosis due to volume depletion
Urine pH>6 because of NH4
+ high synthesis & excretion
NH4
+ low (RTA) & high (Diarrhea)
UAG = [Na+ + K+] u ̶ [Cl-] u estimate NH4
+ Levels
When [Cl-]u > [Na+ + K+]u the UAG (–) suggests extra-renal cause (High urine NH4
+)
If UAG (+) suggests renal cause
Types of RTA:
Classic distal RTA (Type 1):
Hypokalemia, low urine NH4
+ ,
Urine pH>5.5
Hypocitraturia, Hypercalciuria (Nephrolithiasis, Nephrocalcinosis & bone disease)
Proximal RTA (Type 2) the most often:
Manifested by hypokalemia, glycosuria, generalized aminoaciduria & phosphaturia (Fanconi syndrome)
Urine pH<5.5
Therapy by NaHCO3 causes hypokalemia (because HCO3
- not reabsorbed normaly by proximal tubules)
Generalized proximal RTA (Type 3):
Generalized distal RTA (Type 4):
Hyperkalemia (Reduced GFR)
Acommpany with Renal failure (Diabetic nephropathy, Obstructive uropathy & chronic tubulointerstitial disease)
Concurrent HTN & CHF
19. Clinic:
Acute:
Hypercapnea (Tachypnea)
Anxiety
SOB
Confusion
Psychosis
Hallucinations
Coma
Chronic:
Sleep disturbance
Loss of memory
Daytime somnolence
Personality changes
Impairment of coordination
Motor disturbances (Tremor, Myoclonic jerks & Asterixis)
Headaches, Papilledema, abnormal reflexes & focal muscle weakness (secondary loss of co2
vasodilator effects)
Treatment:
Restore adequate alveolar ventilation (Oxygen 2-4Lit/min, Intubation & Mechanical ventilation)
Avoid rapid ventilation correction (Oxygen > 4Lit/min)
Overcorrection leads to Alkalosis (Arrhythmias, Cerebral hypo perfusion & Seizures)
Chronic type is difficult to correct
20. Respiratory alkalosis:
HCO3
- (Low)
Paco2 (Low)
pH (High)
Types:
Acute:
Hypocapnea (Hypoxemia)>2-6 hrs. till renal compensation activates
Full renal adaptation takes several days
Intracellular shifts of (Na+, K+ & PO4
-2)
Reduce free Ca+2 (increase protein-bound fraction)
Hypocapnea- induced hypokalemia is usually minor
No increased HCO3
- renal excretion
DDx with APE, CAD & Hyperthyroidism
Chronic:
Most common in (ICU) & during mechanical ventilation
Occurs in many cardiopulmonary disorders (early to intermediate stages)
Rapid respiratory failure
Hypocapnea (No hypoxemia)
Causes:
CNS stimulation: (Pain, Anxiety/Psychosis, Fever, CVA, Meningitis/Encephalitis, Tumor & Trauma)
Tissue hypoxia/Hypoxemia: (High altitude, Pneumonia/Pulmonary edema, Aspiration & Severe anemia)
Drugs/Hormones: (Pregnancy/Progesterone, Salicylates the most common & HF)
Chest receptors stimulation: (Hemothorax, Flail chest, HF & APE)
Miscellaneous: (Septicemia, Hepatic failure, Mechanical hyperventilation, Heat exposure & Recovery from metabolic acidosis)
21. Clinic:
Dizziness, Confusion & Seizures (Rapid decline in Paco2 )
Arrhythmia occurs due to oxygen unloading in patients with cardiac disease (Bhor effect )
Paresthesia, circumoral numbness, Chest tightness/pain, dizziness, SOB & Tetany (Hyperventilation syndrome)
Thyrotoxicosis, High caloric load & exercise (Precipitants)
Common feature of pregnancy
Prominent in Hepatic failure
Often in gram-negative septicemia
Treatment:
Correct underlying disorder
Reassurance, Rebreathe from a paper bag (Hyperventilation syndrome)
Avoid Antidepressants & Sedatives
To ameliorate hyper adrenergic states use β-blockers
