SEVERE ANEMIA
Patients who have marked loss of red blood cell mass
by hemorrhage, hemolysis, or aplasia run the risk of lacking adequate oxygen
carrying capacity by blood. The more quickly the severe anemia develops, the
less tolerant the patient may be of the insult.
Hemoglobin (Hgb), a powerful carrier for oxygen, carries 1.38 ml of oxygen per gram. The
amount of oxygen that will dissolve in one milliliter of plasma is 0.003 ml per
mmHg of the partial pressure of oxygen (O2) in inhaled gas. CaO2
and CvO2 respectively represent the arterial or venous content of
oxygen in blood. The formula for determination of arterial oxygen content is
given as follows:(1)
CaO2 = (grams Hgb x 1.38 ml O2 x % O2 Hgb)
+ (0.003 + O2 x mm pO2)
Oxygen delivery (DO2) is
calculated by multiplying arterial O2 content by cardiac index
(CI) and is given by the following
formula:(2)
CI = cardiac output (CO) ÷ m2
body surface area (BSA)
DO2 = CI x CaO2
Oxygen consumption (VO2)
is calculated by the Fick equation given by the following formula:(3)
VO2
= CO (CaO2 – CvO2)
On the average, the body extracts 5 to 6 ml of O2
for every 100 ml of blood that sweeps through the microvasculature of most
organ systems. Physiologic normal levels of Hgb readily supply tissue oxygen
extraction rates of 5 to 6 volume percent. As Hgb drops to 6 g/dL, oxygen
delivery, to offset these baseline oxygen extraction rates, becomes problematic
and is clearly inadequate at Hgb levels below 3.6 g/dL.
Accumulative oxygen debt is defined as the time
integral of the VO2 measured during and after shock insult minus the
baseline VO2 required during the same time interval. Clinical
research in evaluation of patients with severe hemorrhage, demonstrates no
chance of survival if the accumulative oxygen debt exceeds 33 L/m2.
Multiorgan failure (MOF) occurs if the accumulative oxygen debt exceeds 22 L/m2.
All patients who have an accumulative oxygen debt of 9 L/m2 survive
without residual disability.(4)
Clinical
Setting
Inability to transfuse red blood cells (RBCs) in
severe anemia occurs when the patient refuses blood upon religious grounds or
if the patient cannot be crossmatched to receive blood. Transfusion-transmitted
infection (TTI), while statistically now less likely with nucleic acid testing
(NAT) [approaches 1 per 2,000,000 units transfused for both human
immunodeficiency (HIV) and hepatitis C (HCV)], still prompts patients to
exercise their right to refuse transfusion.(5)
Untoward inflammatory and immunomodulatory effects
of large RBC transfusions may also be a reason to seek alternatives.(6,7) Blood substitutes, by way of use of
perfluorocarbons or cell wall free polymerized Hgb are still undergoing
randomized clinical trials. While both approaches demonstrate advantages as
well as disadvantages, neither have yet had final FDA approval for routine
clinical uses.(8) Both approaches are still
compatible with adjunctive hyperbaric oxygen (HBO2) therapy. HBO2
therapy for severe anemia has had a long-standing approval for use by the
Centers for Medicare and Medicaid Services (CMS) and its predecessor, the
Healthcare Financing Administration (HCFA).(9,10)
Pulsed HBO2 therapy provides a way to
clinically rectify accumulating oxygen debt in severe anemia when transfusion
is not possible. The patient initially can be placed at treatment pressures of
2.0 to 3.0 ATA or 0.2 to 0.3 Mpa (million pascals) of
oxygen with air breaks for up to three or four hours with surface interval
titrated to avert symptoms associated with reoccurring oxygen debt. Occurrence
of end organ dysfunction (altered mental status, ischemic EKG change,
sprue-like diarrhea from ischemic bowel, hypotension, diminished urinary
output, etc) also may be used as guidance, but are less desirable as their
advent represents more progressed end points of illness or injury. By
adjunctive use of hematinics, the surface intervals between HBO2
treatments can be lengthened gradually until the patient’s baseline Hgb builds
to allow for proper O2 delivery.(11)
Role Of Hyperbaric
Oxygen Therapy
The two most prodigious oxygen using, mammalian
organ systems are the heart and the brain. Oxygen extraction rates of these
systems based on patient activity are 6 ml of O2 per 100 ml of
circulated blood in the brain and 10-20 ml of O2 per 100 ml of
circulated blood in the heart.(12)
As early as 1959, Boerema demonstrated that swine
which were exchanged transfused with 6% dextran/dextrose/Ringers’ lactate
solutions to produce Hgb levels of 0.4 to 0.6 g/dL could survive in the
short-term if they underwent assisted O2 ventilation in a hyperbaric
chamber at 0.3 MPa.(13) HBO2 therapy has
repeatedly allowed survival in what would have otherwise clearly been
unsurvivable clinical circumstance without blood transfusion.
HBO2 therapy provides a way in
severe anemia to successfully correct accumulating oxygen debt in
untransfusible patients.(14)
Evidence Based
Evaluation of Hyperbaric Oxygen Therapy by the Undersea & Hyperbaric
Medical Society’s Hyperbaric Oxygen Committee Standard Approval Criteria
In medical resuscitative intervention, the American
Heart Association (AHA) evidence based criteria is wisely accepted to guide
clinical therapeutic intervention.(15) Normobaric oxygen (NBO2)
is considered a class I indication while HBO2 may be a class II.b.
indication. Controlled animal studies support this assumption as referenced in
the following table:
Evidence-Based Evaluation
(29 studies found for review)
|
|
AHA
|
NCI-PDQ
*
|
BMJ
**
|
|
Level
|
Class
|
NA
|
NA
|
|
6a (16-37) (decisive control groups)
|
II.b.
(acceptable and useful) (16-27)
(29-30) (34-37)
Indeterminate(28, 31, 32, 33)
|
|
6b(38-43) (not decisive control group)
|
II.b.
(acceptable and useful)(38,39,40)
|
|
|
Indeterminate(41, 42, 43, 44)
|
|
|
|
|
|
* National Cancer Institute Patient Data
Query evidence-based criteria (NCI-PDQ)(45)
** British Medical Journal evidence-based
criteria (BMJ)(46)
Rather consistently this body of literature confirms
over and over again better survival in animal models of both hemorrhage to a
predetermined mean arterial pressure (Wiggers model)(47) or fixed volume hemorrhage.(48) Both increased short-term
and long-term survival for HBO2 groups over normobaric air (NBA) or
NBO2 groups.
Published human case reports and case series allow
similar evidence-based acceptance. Published case reports or case series are
referenced below for tabulated uniform approval:
|
|
|
AHA
|
NCI-PDQ
|
BMJ
|
|
Level
|
Class
|
3.iii.
(case series or presentation neither consecutive or population based)(11,49-53,55,56)
|
Most
likely beneficial(11, 49-53, 55,
56)
|
|
5
(case series and case reports)
|
II.b.
(acceptable and useful)(53)
Indeterminate
(11,49-52,55,56)
|
|
6
|
II.b.
(54)
|
NA
|
NA
|
(A more detailed repots of the above tabulated
findings has been published in a focused journal review article on the use of
HBO2 in acute blood loss anemia)(57)
In summary, both by the support of animal work
and human clinical experience evidence-based analysis firmly supports the use
of HBO2 as a treatment option in severe anemia using AHA, NCI-PDQ,
and BMJ evidence-based criteria.
______________________
More Information and References can be found
in the 12th Edition of the Hyperbaric Oxygen Therapy Indications
Book. For Sale on
the UHMS
Publications page.