What causes a right shift in the oxygen-hemoglobin dissociation curve?

Right shift is caused by increased CO2, decreased pH (acidosis), increased 2,3-BPG, increased temperature, and vigorous exercise. The mnemonic CADET helps: CO2, Acid, 2,3-DPG, Exercise, Temperature. Right shift means lower O2 affinity, which helps release oxygen to working tissues.

What is the difference between HbF and HbA oxygen affinity?

Fetal hemoglobin (HbF) has lower affinity for 2,3-BPG than adult HbA. Because 2,3-BPG normally reduces O2 affinity, HbF (which ignores it) has higher O2 affinity. This allows HbF to pull oxygen from maternal HbA across the placenta.

Why does carbon monoxide cause a left shift on the dissociation curve?

Carbon monoxide binds hemoglobin about 200 times more strongly than oxygen and causes an allosteric conformational change that shifts the remaining unbound subunits into the R-state (high affinity). This left shift means the remaining bound O2 is held too tightly and cannot be released to tissues.

What is the P50 of normal adult hemoglobin?

Normal adult hemoglobin has a P50 of approximately 26 mmHg. This is the partial pressure of oxygen at which hemoglobin is 50 percent saturated. Right shift increases P50 (less affinity); left shift decreases P50 (more affinity).

Why is the pulse oximeter unreliable in CO poisoning and methemoglobinemia?

Standard pulse oximetry uses two wavelengths and cannot tell oxyhemoglobin from carboxyhemoglobin, so it reads falsely high in CO poisoning. Methemoglobin absorbs at both wavelengths and drags the reading toward 85 percent. Both require co-oximetry on a blood gas for the true value.

Hemoglobin and O2 Dissociation Curve

Hemoglobin T-state to R-state conformational change animation

Sickle cell anemia blood smear with crescent shaped red cells

Chocolate brown blood of methemoglobinemia next to normal red blood

Howell-Jolly body inside a red blood cell on peripheral smear

The Numbers That Win Points

pO2 = 60 mmHg= 90% saturation (the knee)

P50 (normal HbA)= 26 mmHg

CO vs O2 affinityCO binds about 200x stronger

HbA: 2alpha + 2beta98% of adult Hb

HbF: 2alpha + 2gammaleft shift (ignores 2,3-BPG)

Cooperative Binding: Watch T-state Relax to R-state

Press Bind next O2. Each oxygen flies into a heme, the cooperative wave sweeps the tetramer, and the whole molecule slides from tense and clamped (left) toward relaxed and high-affinity (right). That allosteric switch is why the curve is sigmoid.

T-state, zero O2: all four subunits tense and clamped. Low affinity. This is hemoglobin arriving in oxygen-poor tissue.

O2-Hemoglobin Dissociation Curve

The S-shape is cooperative binding made visible. Tap each curve to see what shifts it clinically.

Structure: The Hemoglobin Tetramer ▼

Hemoglobin is a quaternary protein: 4 globin chains, each hugging one heme group, each heme carrying one iron (Fe2+) that grabs one O2. Total capacity: 4 O2 per molecule.

Tap a blurred cell, or use the button, to self-test the tetramer table.

Type	Subunits	Context	Curve
Hb A	2alpha + 2beta	98% adult	Normal
Hb A2	2alpha + 2delta	2% adult	Normal
Hb F	2alpha + 2gamma	Fetal / neonates	Left shift
Hb S	2alpha + 2beta(E6V)	Sickle cell	Normal P50; polymerizes when deoxy

Memory hook · tap to reveal Alpha chains are present in ALL types. The beta, gamma, or delta chain is what defines each variant. Hb A = Alpha Beta = Adult.

The key board fact: myoglobin is a MONOMER (1 chain, 1 heme). It has a hyperbolic curve (not sigmoid) because it cannot do cooperative binding. Highest O2 affinity of any oxygen-binding protein. It is the muscle oxygen reserve.

Right Shift: CADET, Face Right ▼

Right shift means lower O2 affinity: hemoglobin gives up oxygen more easily to tissues. P50 rises above 26 mmHg.

Memory hook · tap to reveal CADET (face right for right shift): CO2 up · Acidosis (H+ up) · DPG (2,3-BPG) up · Exercise · Temperature up

The Bohr effect is the pH and CO2 piece: when CO2 rises in tissues, H+ rises, hemoglobin binds H+ and releases O2 to the tissues that are actually working. This is purposeful physiology, not a failure.

2,3-BPG is produced in RBCs during glycolysis. It stabilizes the T-state (deoxy conformation), shifting the curve right. Chronically hypoxic patients (high altitude, chronic anemia) upregulate 2,3-BPG as an adaptation to deliver more O2 despite lower Hb levels.

From the Attending

The board favorite: a patient with chronic anemia, Hgb 7, but surprisingly comfortable. The question is asking you to explain why. The answer is compensatory 2,3-BPG elevation causing a right shift. Low Hb does not always mean a sick patient: the curve adapts.

Quick self-test: list all five CADET right-shift factors before revealing.

Left Shift: HbF, CO, Methemoglobin, Alkalosis ▼

Left shift means higher O2 affinity: hemoglobin holds onto O2 too tightly and refuses to release it to tissues. P50 falls below 26 mmHg.

Memory hook · tap to reveal FALCO: Fetal Hb · Alkalosis · Low temperature · CO poisoning · Other (methemoglobin)

Tap a blurred cell, or use the button, to self-test the left-shifters.

Agent	How it shifts left	Board tell
HbF	Gamma chains ignore 2,3-BPG; HbF stays in R-state (high affinity)	Neonate; shifts to HbA by 6 months
CO	About 200x O2 affinity; allosteric lock into R-state for remaining subunits	Cherry red skin; SpO2 falsely normal
MetHb	Fe3+ cannot bind O2; remaining Fe2+ sites are locked in high-affinity state	Cyanosis with normal PaO2; chocolate blood
Alkalosis	Low H+ reduces Bohr effect; Hb holds O2 more tightly	Hyperventilation patient, CXR normal

CO poisoning board trap: pulse oximetry reads falsely normal (it cannot tell HbO2 from HbCO). The patient is dying with a 99% saturation. Always order a co-oximeter ABG when CO poisoning is suspected, not a standard pulse ox.

Methemoglobin board trap: SpO2 is low (78 to 85%) but PaO2 on ABG is normal. Treatment: methylene blue 1 to 2 mg/kg IV. It reduces Fe3+ back to Fe2+ via the NADPH pathway. Watch for G6PD-deficient patients: methylene blue fails (they cannot generate NADPH), and exchange transfusion is required instead.

HbA vs HbF vs HbS: The Tale of Three Tetramers

Same alpha chains, three different partners. Tap a fighter to see what makes it behave.

HbA: the adult workhorse

Subunits2 alpha + 2 beta

Share of adult HbAbout 98%

P5026 mmHg (normal)

2,3-BPG bindingStrong: tunes delivery

Board hookThe reference curve everything else shifts off

HbF: the placental thief

Subunits2 alpha + 2 gamma

2,3-BPG bindingPoor: stays in R-state

CurveLeft shift, higher affinity

Why it mattersPulls O2 off maternal HbA across the placenta

Board hookReplaced by HbA by 6 months; protects newborns with HbSS

HbS: one swap, a career ruined

Subunits2 alpha + 2 beta with Glu6Val

P50Roughly normal at baseline

The catchDeoxy HbS polymerizes; cells sickle

TriggersHypoxia, acidosis, dehydration, fever, cold

Board hookHydroxyurea raises HbF, which cannot join the polymer

The Blue Patient: A Discriminator

A patient looks dusky or the pulse ox is low. Commit to an answer at each step, then reveal the logic. CO, methemoglobin, and anemia all read differently if you know where to look.

Step 1 of 3

The pulse oximeter reads LOW, but the arterial blood gas PaO2 comes back NORMAL. What does that mismatch tell you?

Step 2 of 3

You draw blood. It is CHOCOLATE BROWN and does not turn red when shaken in air. SpO2 is stuck near 85%. Which carrier problem is this?

Step 3 of 3

Methemoglobin is confirmed and the child is symptomatic. What is the first-line antidote, and what one detail would change your plan?

O2 Content vs pO2 vs Saturation: The Triple Confusion ▼

O2 content (mL O2/dL blood) = (1.34 x Hgb x SaO2) + (0.003 x PaO2)

The 0.003 term (dissolved O2) is tiny. Almost all O2 is carried by hemoglobin. This means:

Anemia: Hgb is low, O2 content is low, but PaO2 is NORMAL. This is not hypoxemia. The lungs are fine.
CO poisoning: PaO2 is normal (dissolved O2 is unaffected). SpO2 is normal (pulse ox fooled). O2 content is catastrophically low (Hb occupied by CO).
Polycythemia: Hgb is high, O2 content is high. Useful at altitude.

Board stems love to present CO poisoning with a normal pulse ox and ask why the patient is dying. The O2 content equation is the answer: it is carrying capacity, not partial pressure, that fails.

Fetal Hemoglobin and the Placental Gradient ▼

In the placenta, maternal and fetal blood run side by side but do not mix. Fetal hemoglobin needs to pull oxygen off maternal HbA, and a steeper left-shift is the mechanism.

HbF gamma chains bind 2,3-BPG poorly. Because 2,3-BPG normally stabilizes the T-state (reduces affinity), HbF without BPG binding stays in R-state: high affinity. Maternal HbA, which does bind BPG, has lower affinity. O2 moves from mother to fetus along this gradient.

Memory hook · tap to reveal HbF = BPG-independent = always R-state = high affinity = left shift. This cannot release O2 to tissues efficiently: fine for a fetus getting O2 from mom, fatal for an adult needing tissue delivery.

Hydroxyurea induces HbF production in sickle cell patients. HbF chains cannot participate in HbS polymerization (which requires beta chains with valine at position 6). More HbF means fewer sickling events. Trade-off: bone marrow suppression (check the CBC).

Physiologic timeline: HbF peaks at birth and falls to adult levels (less than 1%) by 6 months. Neonates with sickle cell disease are asymptomatic at birth because of high HbF. Symptoms emerge as HbF wanes after 6 months: the classic dactylitis presentation.

Sickle Cell Disease: Mechanism to Crisis ▼

The mutation: beta-globin position 6, glutamic acid (hydrophilic) replaced by valine (hydrophobic). One hydrophobic swap ruins a career.

When O2 is present, valine is pulled toward the protein exterior by the conformational change and the RBC stays round. When O2 falls, valine sinks hydrophobically into adjacent HbS molecules, forming rigid polymers: crescent shape, vessel occlusion.

Triggers of sickling: hypoxia, acidosis, dehydration, fever, infection, cold exposure, and high altitude. The board will present one of these as the precipitant.

Tap a blurred cell, or use the button, to self-test the complications.

Complication	Underlying process	Key board fact
Dactylitis	Vaso-occlusion in hand and foot vessels	First manifestation after 6 months
Acute chest syndrome	Pulmonary vaso-occlusion plus infection	Most common cause of death
Aplastic crisis	Parvovirus B19 infects erythroid progenitors	Reticulocyte count falls to near zero
Autosplenectomy	Repeated splenic infarcts by age 6	Howell-Jolly bodies on smear
Splenic sequestration	Sudden pooling in spleen	Rapid fall in Hgb, shock
Avascular necrosis	Femoral or humeral head infarction	Hip pain with normal plain film early

Management: acute crisis gets O2, IV fluids, and analgesics (opioids for severe pain). CVA gets exchange transfusion (not tPA, not aspirin: this is mechanical, not thrombotic). Aplastic crisis gets supportive care and transfusion if severe; the Parvovirus infection is self-limited. Prophylaxis: pneumococcal, meningococcal, and Hib vaccines, plus penicillin prophylaxis through age 5.

From the Attending

Aplastic crisis: the classic board setup is a sickle cell child with fever and rash 2 to 3 weeks ago, now profoundly anemic. The rash was slapped-cheek from Parvovirus B19. The reticulocyte count is the key lab. If it is near zero, the marrow has shut down, so this is not sickling and not sequestration. Anemia plus a near-zero reticulocyte count after a slapped-cheek illness is aplastic crisis until proven otherwise.

Board-Style Walkthrough

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Hemoglobin & O2 Dissociation