What is the primary mechanism by which digoxin improves symptoms in heart failure?

Increases intracellular calcium levels

Which of the following would cause an immediate reduction in the amount of potassium leaking out of a cell?

Hyperpolarizing the membrane potential

Reducing the activity of the sodium-potassium pump

Decreasing the extracellular potassium concentration

Increasing the permeability of the membrane to potassium

What is the PRIMARY mechanism by which the Na+-Ca2+ exchanger functions in cardiac muscle cells?

Na+-Ca2+ exchanger acts to remove Ca2+ from heart muscle cells

Na+-Ca2+ exchanger requires ATP directly

The Na+-Ca2+ exchanger operates in reverse mode during normal cardiac contraction

The Na+-Ca2+ exchanger primarily moves Ca2+ into cardiac muscle cells during systole

Which of the following is the primary mechanism that drives sodium reabsorption in the proximal tubule?

Active sodium transport via the Na+-K+-ATPase pump at the basolateral membrane.

Sodium reabsorption through cotransport with amino acids at the luminal membrane.

Sodium reabsorption through cotransport with glucose at the luminal membrane.

Sodium reabsorption through countertransport with hydrogen ions at the luminal membrane.

Which of the following is true regarding Na+ (sodium) ions?

Does not help other ions in transport

Responsible for the resting membrane potential

Sodium ion is responsible for Donnan effect

Sodium-Potassium ATPase for FMGE: High-Yield Biochemistry Lessons

Na⁺/K⁺ ATPase Basics - Pump It Up!

Definition: An active transporter enzyme crucial for maintaining electrochemical gradients across the plasma membrane.
Type: P-type ATPase (forms a phosphorylated intermediate).
Location: Ubiquitous in animal cell plasma membranes.
Stoichiometry & Energy: Pumps $3 Na^+{out} / 2 K^+{in}$ per ATP hydrolyzed.

⭐ The Na⁺/K⁺ ATPase is specifically inhibited by cardiac glycosides like digoxin and ouabain, which bind to the extracellular K⁺ site (E2-P form).

Pump Structure - The Molecular Machine

Heterodimer: α and β subunits.
- α-subunit: Catalytic; binds 3 Na⁺, 2 K⁺, ATP. Has phosphorylation & cardiac glycoside (e.g., ouabain) sites.
- β-subunit: Glycosylated; aids α-subunit maturation & correct membrane insertion. Stabilizes α-subunit.

Na,K-ATPase alpha and beta subunit assembly and trafficking

⭐ The α-subunit houses all key functional sites: ion (Na⁺, K⁺) and ATP binding, phosphorylation, and cardiac glycoside interaction.

Mechanism Unveiled - The Pump Cycle

The Na⁺/K⁺-ATPase, a P-type ATPase, operates via the Post-Albers cycle, alternating between E1 (cytosolic) and E2 (extracellular-facing) conformations.

E1 State (Cytosolic facing):
- High Na⁺ affinity; binds ATP & 3 Na⁺ from cytosol.
- $E1 + ATP + 3Na^+_{in} \rightarrow E1 \cdot ATP \cdot 3Na^+$
Phosphorylation $\rightarrow$ E1~P:
- ATP hydrolysis: $E1 \cdot ATP \cdot 3Na^+ \rightarrow E1\text{\textasciitilde}P \cdot 3Na^+ + ADP$.
- Conformational change to E2-P (Na⁺ translocated out).
- $E1\text{\textasciitilde}P \cdot 3Na^+ \rightarrow E2\text{\textasciitilde}P \cdot 3Na^+$
E2-P State (Extracellular facing):
- Releases 3 Na⁺ to extracellular space: $E2\text{\textasciitilde}P \cdot 3Na^+ \rightarrow E2\text{\textasciitilde}P + 3Na^+_{out}$.
- High K⁺ affinity; binds 2 K⁺ from extracellular space.
- $E2\text{\textasciitilde}P + 2K^+_{ext} \rightarrow E2\text{\textasciitilde}P \cdot 2K^+$
Dephosphorylation (K⁺ dependent) $\rightarrow$ E2:
- $E2\text{\textasciitilde}P \cdot 2K^+ \rightarrow E2 \cdot 2K^+ + P_i$.
- Conformational change to E1 (K⁺ translocated in).
- $E2 \cdot 2K^+ \rightarrow E1 \cdot 2K^+$
- Releases 2 K⁺ to cytosol: $E1 \cdot 2K^+ \rightarrow E1 + 2K^+_{in}$.

📌 Mnemonic: KIN (K⁺ In), NAO (Na⁺ Out). Pumps 3 Na⁺ Out, 2 K⁺ In.

Sodium-Potassium ATPase pump cycle

⭐ Cardiac glycosides (e.g., Digoxin) inhibit Na⁺/K⁺-ATPase by binding to the E2-P (phosphorylated) form on its extracellular side.

Pump's Purpose - Cellular Gatekeeper

Maintains resting membrane potential (RMP), crucial for nerve and muscle cell excitability.
Regulates cell volume by controlling intracellular solute concentration, preventing osmotic lysis or crenation.
Drives secondary active transport for solutes like glucose and amino acids (e.g., Na⁺-glucose cotransport) and ions (e.g., Na⁺/Ca²⁺ exchange).
Establishes and preserves steep electrochemical gradients for $Na⁺$ (low inside) and $K⁺$ (high inside).

Sodium-Potassium Pump Mechanism

⭐ The pump transports 3 $Na⁺$ ions out of the cell and 2 $K⁺$ ions into the cell for each molecule of ATP hydrolyzed, making the inside of the cell negative relative to the outside (electrogenic effect).

Pump Control - Who's the Boss?

Short-term:
- Substrate availability: Intracellular $Na^+$ ([Na⁺]i), extracellular $K^+$ ([K⁺]o), ATP.
Long-term:
- Hormonal control: Insulin ↑, Aldosterone ↑, Thyroid hormones ↑ activity/synthesis.
- Covalent modification: Primarily via phosphorylation by PKA/PKC, altering pump activity.
- Endogenous regulators: e.g., endogenous ouabain-like substances.

⭐ Insulin promotes $Na^+$-$K^+$ ATPase activity, driving $K^+$ into cells, which can cause hypokalemia.

Clinical Angles - When Pumps Fail

Inhibitors: Cardiac glycosides (e.g., Digoxin).
- Bind E2-P form, block dephosphorylation → ↑ [Na⁺]i → reverses Na⁺/Ca²⁺ exchanger → ↑ [Ca²⁺]i → ↑ contractility.
Digoxin:
- Uses: Heart failure, atrial fibrillation. Therapeutic range: 0.5-0.9 ng/mL.
- Toxicity: 📌 BEWS (Blurred vision/yellow halos, EKG changes, Weakness, Stomach upset).
K⁺ Levels: Hypokalemia ↑ Digoxin toxicity; Hyperkalemia ↓ efficacy.

Digitalis effect on Na/K ATPase and cardiac inotropy

⭐ Hypokalemia potentiates Digoxin toxicity by increasing its binding to the Na⁺/K⁺-ATPase pump, leading to enhanced effects and risk of adverse events.

High‑Yield Points - ⚡ Biggest Takeaways

A P-type ATPase crucial for active ion transport across plasma membranes.

Establishes ion gradients by pumping 3 Na+ out and 2 K+ in.

Utilizes one ATP molecule per transport cycle for energy.

Maintains resting membrane potential, cell volume, and drives secondary active transport.

Specifically inhibited by cardiac glycosides (e.g., Digoxin, Ouabain).

Its activity is electrogenic, contributing to the negative intracellular potential an_average_of_-10mV_to_the_RMP_in_neurons

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