Renal Recap

Question 1

Label the Nephron

Answer 1

Question 2

What is the difference between the Principal Cells and Intercalated Cells in the CD?

Answer 2

Principal cells have a few mitochondria, mostly function for NaCl reabsorption and K secretion.
Intercalated cells have a lot of mitochondria and function in acid-base regulation. Some IC secrete H+, some secrete HCO3-

Question 3

What is the structure of the juxtaglomerular apparatus?

Answer 3

macula densa of thick ascending LH + extraglomerular mesangial cells + granular cells of afferent arteriole (manufacture, store, and secrete renin)

Question 4

What is the function of the juxtaglomerular apparatus?

Answer 4

sense Na/pressure, involved in autoregulation of renal blood flow, GFR, systemic BP control

Increase in afferent arteriole pressure 🡪 increased glomerular pressure 🡪 increased GFR.
Increased Na/K delivery to macula densa 🡪 decreased renin. And viceversa.

Question 5

Within what range of systemic BP is the (healthy) kidney able to provide auto-regulation of renal blood flow?

Answer 5

80-180 mmHg

Question 6

What happens to renal blood flow and GFR with dilation of the afferent arteriole?

Answer 6

RBF: up
GFR: up

Question 7

What happens to renal blood flow and GFR with Constriction of the afferent arteriole?

Answer 7

RBF: down
GFR: down

Question 8

What happens to renal blood flow and GFR with Dilation of the efferent arteriole?

Answer 8

RBF: up
GFR: down

Question 9

What happens to renal blood flow and GFR with constriction of the efferent arteriole?

Answer 9

RBF: down
GFR: up

Question 10

Name the 3 main renal transport mechanisms:

Answer 10

1. Passive transport (diffusion)
2. Active transport
3. Endocytosis

Question 11

Describe passive transport (diffusion)

Answer 11

Movement down a concentration gradient or electrical gradient.

Includes solvent drag (movement of ions with water even if not with concentration gradient) and Facilitated diffusion (passive, but requires transport protein- uniport, smport, antiport, or secondary active transport)

Question 12

Describe Active transport

Answer 12

coupled directly with energy (ATP)

Question 13

Describe endocytosis

Answer 13

movement by invagination of plasma membrane, does require ATP

Question 14

Draw and explain the basic mechanisms of electrolyte reabsorption/secretion in the kidneys.
This does not have to be a specific site or electrolyte.

Answer 14

1. Active transport at the basolateral membrane (3Na/2K/ATPase pump) creates a gradient (Na out of cell into interstitium, K into cell)
2. Passive transcellular transport at the luminal membrane driven by concentration gradient, partially created by the active pump (cotransporters, antitransporters) and partially created due to lower concentration of electrolytes in blood (highly filtered at glomerulus)
3. Paracellular transport driven by transepithelial (transmembrane) potential difference (electrical charge)- lumen positive or lumen negative
   Paracellular solute drag along with water (aids with reabsorption)
4. “Sink” effect from rapid tubular flow (aids excretion)

Question 15

What is the PRIMARY function of the proximal tubule?

Answer 15

reabsorption of most water (67%) and solutes (Na, Cl, K, glucose, AA’s) linked to Na/K ATP-ase pump in basolateral membrane

Question 16

What is the PRIMARY function of the thin descending LH?

Answer 16

H20 reabsorption through aquaporins with NO NaCl

Question 17

What is the PRIMARY function of the thin ascending LH?

Answer 17

Na/Cl reabsorbed through passive diffusion, NO H20

Question 18

What is the PRIMARY function of the Thick ascending LH?

Answer 18

Reabsorption of solutes via Na/K/ATPase in basolateral membrane. NO H20. “Diluting segment”- solutes out of tubule, H2O stays in.

Question 19

What is the PRIMARY function of the distal tubule?

Answer 19

“Adjustment” of lytes but impermeable to H20

Question 20

What is the PRIMARY function of the late distal tubule and the CD?

Answer 20

Principal cells: reabsorb Na/H2O, secrete K

Intercalated cells:
— α-intercalated cells secrete H+, reabsorb HCO3- and K+
— β-intercalated cells secrete HCO3-, reabsorb H+ and Cl-

Question 21

Angiotensin II:

Major stimulus:
Nephon site of action:
Effect on transport:

Answer 21

Major stimulus: ↑ Renin

Nephon site of action:
Proximal tubule
Thick ascending limb
Distal tubule /Collecting duct

Effect on transport: ↑ NaCl and H2O reabsorption

Question 22

Aldosterone

Major stimulus:
Nephon site of action:
Effect on transport:

Answer 22

Major stimulus: ↑ Angiotensin II
↑ [K+]p

Nephon site of action:
Thick ascending limb
Distal tubule /Collecting duct

Effect on transport: ↑ NaCl and H2O reabsorption

Question 23

ANP, BNP, urodilatin

Major stimulus:
Nephon site of action:
Effect on transport:

Answer 23

Major stimulus: ↑ ECFV

Nephon site of action: Collecting duct

Effect on transport: ↓ H2O and NaCl reabsorption

Question 24

Uroguanylin, guanylin

Major stimulus:
Nephon site of action:
Effect on transport:

Answer 24

Major stimulus: Oral ingestion of Nacl

Nephon site of action:
Proximal tubule
Collecting duct

Effect on transport: ↓ H2O and NaCl reabsorption

Question 25

Sympathetic nerves

Major stimulus:
Nephon site of action:
Effect on transport:

Answer 25

Major stimulus: ↓ ECFV

Nephon site of action:
Proximal tubule
Thick ascending limb
Distal tubule /Collecting duct

Effect on transport:↑ NaCl and H2O reabsorption

Question 26

Dopamine

Major stimulus:
Nephon site of action:
Effect on transport:

Answer 26

Major stimulus: ↑ ECFV

Nephon site of action: Proximal tubule

Effect on transport: ↓ H2O and NaCl reabsorption

Question 27

ADH/AVP

Major stimulus:
Nephon site of action:
Effect on transport:

Answer 27

Major stimulus:
↑ Posm
↓ ECFV

Nephon site of action: Distal tubule /Collecting duct (aquaporins)

Effect on transport:↑ H2O reabsorption

Question 28

Briefly explain RAAS

Answer 28

• Juxtaglomerular cells in the afferent arterioles synthesize and secrete renin
• Renin secretion is stimulated when:
  – Perfusion pressure to the kidneys is reduced
  – Sympathetic innervation to the kidneys is activated
  – NaCl delivery to the macula densa is decreased
• Renin converts Angiotensinogen (produced by liver) 🡪 Angiotensin I
  – AT I 🡪 AT II by ACE in the kidneys and lungs
  – AT II stimulates aldosterone secretion, vasoconstricts arterioles, stimulates ADH + thirst, and enhances NaCl reabsorption by the kidneys

Question 29

What is the primary regulator of K secretion in the kidney?

Answer 29

Aldosterone

Question 30

Define Net endogenous Acid production (NEAP)

Answer 30

The production of non-volatile acid to the body daily.

Due to diet, cellular metabolism, and the loss of bicarbonate in the feces.

Question 31

Define Renal Net Acid Secretion

Answer 31

The amount of acid secreted by the kidney per day, typically equal to the NEAP

Question 32

What are the 2 main buffer systems in the kidney that lead to formation of new HCO3?

Answer 32

Phosphate and Ammonia

Question 33

What is the expected compensatory response for metabolic acidosis?

Answer 33

0.7 decrease in pCO2 for every 1mEq decrease in HCO3

Question 34

What is the expected compensatory response for metabolic alkalosis?

Answer 34

0.7 increase in pCO2 for every 1mEq increase in HCO3

Question 35

What is the expected compensatory response for respiratory acidosis?

Answer 35

Acute: 0.15 increase HCO3 for 1mmHg pCO2

Chronic: 0.35 increase HCO3 for 1mmHg pCO2

Question 36

What is the expected compensatory response for respiratory alkalosis?

Answer 36

Acute: 0.25 decrease HCO3 for 1mmHg pCO2

Chronic: 0.55 decrease HCO3 for 1mmHg pCO2

Question 37

What portion(s) of the kidney contain Calcium Sensing Receptors (CaSR’s)?

Answer 37

Thick Ascending LH and Proximal Tubule

Question 38

What is the primary regulator of urinary Calcium excretion?
What effect does this hormone have on calcium and phosphorus?

Answer 38

PTH

• it increases calcium reabsorption (decreases excretion) and increases phosphorus excretion (inhibits reabsorption)

Question 39

Label the following diagram with the diuretic that acts at each site.

Answer 39

1. Diuretic: Furosemide (loop)
2. Diuretic: Thiazides
3. Diuretic: K sparing
4. Diuretic: Osmotic (Mannitol)

Question 40

Explain the net effect of Furosemide (inhibition, stimulation, electrolyte changes in the patient).

Answer 40

• Loop diuretic
• Net effect: inhibits Na/K/2Cl cotransporter, leading to increased loss of Na/K/Cl in urine 🡪 increased water loss.
• MOST POTENT- loop of henle is the main site of creation of the urine concentration gradient

Question 41

Explain the net effect of Thiazides (inhibition, stimulation, electrolyte changes in the patient).

Answer 41

• Net effect: inhibits Na/Cl cotransporter leading to increased Na/Cl and water loss in the urine.
• Less potent because the DCT is mostly for fine tuning (not large volume of electrolyte movement).

Question 42

Explain the net effect of K sparing diuretics (inhibition, stimulation, electrolyte changes in the patient).

Answer 42

• Net effect: block Na channels in the CD (ENaC- amilioride, triamterene) , so less Na reabsorption.
• Aldosterone antagonists (like spironolactone) antagonize the effect of aldosterone on these channels.
• Loss of Na and water, but not K.

Question 43

Explain the net effect of osmotic diuretics (mannitol) (inhibition, stimulation, electrolyte changes in the patient).

Answer 43

Net effect: inability to reabsorb H20 due to osmotic pull into tubule

Question 44

What are the 4 methods of solute/water movement across the dialysis membrane?

Answer 44

Ultrafiltration
Diffusion
Convection
Adsorption

Question 45

Describe Ultrafiltration

Answer 45

movement of water only (either pressure or osmotic)

Question 46

Describe diffusion

Answer 46

solute moves down concentration gradient, small molecules

Question 47

Describe convection

Answer 47

solute moves with drag due to water flow, medium molecules

Question 48

Describe adsoprtion

Answer 48

solute binds to the membrane itself, larger molecules

Question 49

List the indications for renal replacement therapy

Answer 49

Azotemia not responsive to traditional therapy
Severe uremic symptoms
Severe hyperkalemia
Oliguria
Volume overload
Diffusible toxins

Question 50

What is dialysis disequilibrium syndrome?

Answer 50

• Rapid changes in osmolarity (drop in BUN) can lead to fluid shifts into the brain 🡪 cerebral edema, neurologic symptoms, death
• Need to drop BUN slowly at first
• Can prophylactically give mannitol in high-risk patients (BUN >150, < 5kg)
• Can use “sodium profiling” with initially high-sodium dialysate

Question 51

Label the diagram with the 4 different modes of CRRT/hemodialysis.

Answer 51

SCUF - CVVH
CVVHD - CVVHDF

Question 52

Describe SCUF.

Answer 52

= slow continuous ultrafiltration

• No dialysate or replacement fluids
• Just fluid removal (ie CHF)

Question 53

Discuss CVVH.

Answer 53

= continuous veno-venous hemofiltration

• Removal of solutes via convection (also ultrafiltration)
• Needs replacement fluid, no dialysate

Question 54

Discuss CVVHD.

Answer 54

=continuous veno-venous hemodialysis (also ultrafiltration)

• Removal of solutes via diffusion, no convection
• Dialysate only, no replacement fluids

Question 55

Discuss CVVHDF.

Answer 55

= continuous veno-venous hemodiafiltration

• Removal of solutes by diffusion, convection, ultrafiltration
• Dialysate and replacement fluid

Question 56

What are the possible treatment options for obstructive ureteral disease?

Answer 56

• Medical management: IVF, osmotic diuretics, smooth muscle dilators, renal replacement therapy
• Nephrostomy tube (short term)
• Ureterotomy
• Ureteral re-implantation
• Ureteral stenting
• Subcutaneous ureteral bypass
• Renal transplant

Question 57

What percentage of cats with urethral obstruction due to idiopathic causes will reobstruct ever in their lifetime?

Answer 57

33-50% depending on study

Question 58

Debate: is a uroabdomen a surgical emergency?

Answer 58

Yes: can cause significant chemical peritonitis, could be a septic peritonitis (if other internal injuries or if urine was infected), hyperkalemia can be life threatening

No: can divert urine with combination of abdominal and urinary catheter to get patient more stable

Question 59

What are the 4 phases of AKI?

Answer 59

1. Initiation phase
2. Extension phase
3. Maintenance phase
4. Recovery phase

Question 60

Discuss the initiation phase of an AKI

Answer 60

• Intervention may prevent progression to more severe injury.
• Injury is at subcellular level and may not be biochemically evident.

Question 61

Discuss the extension phase of an AKI

Answer 61

• Cellular injury progresses to cell death
• Biochemical derangements and clinical manifestations of disease manifest

Question 62

Discuss the Maintenance phase of an AKI.

Answer 62

• Both cell death and regeneration occur simultaneously
• The potential for and length of recovery may be determined by the balance b/w these processes.
• Removal of inciting cause does not alter existing damage but may allow for balance to shift in favor of parenchymal regeneration.

Question 63

Discuss the recovery phase of an AKI.

Answer 63

• Characterized by improvement of GFR and tubular function
• May last weeks to months.

Question 64

Do fluids fix kidneys? Explain your answer.

Answer 64

Yes: Dehydration and poor perfusion are detrimental to the kidneys. Fluid therapy once re-hydrated and hemodynamically stable can help to replace losses (higher losses if polyuric + insensible losses) to prevent future development of dehydration. Appropriate amounts of fluids are helpful.

No: Fluid overload has been found to be more harmful to the kidneys than being mildly dehydrated. Renal edema worsens urine output. Edema of other organs is also very harmful (ie GI edema- nausea/ileus, cerebral edema, pulmonary edema). More fluids are not better.

Question 65

Explain the basic concept/utility of staging systems for acute kidney injury and name them.

Answer 65

• These are a way to track/identify renal injury in hospitalized patients and aid in prognosis
• Based on single Creat or rise in creat + urine output
• Studies have shown that any rise in creat, even if still within reference range, increases risk of death!
• RIFLE/AKIN (human), VAKI (Veterinary)

Question 66

Why do patients with CKD become anemic? Based on this, what would be ways to treat it?

Answer 66

• Inadequate EPO production, blood loss (uremic ulceration, iatrogenic from sampling), decreased RBC lifespan due to uremic damage, anemia of chronic disease (illness/inflammation related bone marrow suppression, iron deficiency)
• Minimize uremia, antacids, minimize blood draws, hormone supplementation (Darbo preferred to EPO- less anti-EPO-antibody formation)

Question 67

What 3 criteria are used to determine IRIS stage for CKD?

Answer 67

• Degree of azotemia (determined by STABLE Creat)
• Proteinuria
• Hypertension

Question 68

BRIEFLY name/explain the 3 main theories for perpetuation of kidney injury (from canine remnant kidney model)

Answer 68

1. Intact nephron hypothesis: If 1 part of a nephron is damaged, remaining parts degenerate so whole nephron is lost. Remaining intact nephrons hypertrophy to compensate for the increased load (hyperfiltration) which damages them.
2. Hyperfiltration theory: Remaining nephrons are hyperperfused, have hyperfiltration, and glomerular hypertension + glomerular inflammation 🡪 Proteinuria 🡪 nephron damage.

3.Trade-off hypothesis: Phosphorus build up, ionized hypocalcemia 🡪 high PTH levels, low calcidiol/calcitriol levels, high FGF-23 levels 🡪 faster progression of CKD

Question 69

Explain the pathogenesis of renal secondary hyperparathyroidism.

Answer 69

• Loss of nephron mass from chronic disease increase in serum Phos 🡪 increased FGF-23 (which binds to receptor only with the help of his friend Klotho which is present in kidneys and parathyroid gland)
• Phos initially is kept in normal range
• FGF-23 and progressive renal disease both cause decreased calcitriol/calcidiol production 🡪 low iCa 🡪 PTH secretion
• Normalizes iCa but also increases serum Phos (and PTH is now increased)
• Worsening GFR/hyperphosphatemia 🡪 further increase in FGF-23 and further decreases in calcitriol/calcidiol 🡪 worsening hypocalcemia, continual increase in PTH, Phos also gets much worse because FGF-23 stops working (not enough tubules, not enough receptors)
• Chronic bone reabsorption 🡪 loss of bone mass
• This whole process speeds up progression of CKD

Question 70

List the most effective ways to slow the progression of CKD

Answer 70

• Renal diet (phosphorus limited + fatty acids/antioxidants, also low protein which is less important)
• Phosphate binders if not controlled enough with diet
• Calcitriol supplementation
• Mimimize proteinuria and glomerular hypertension (ACE inhibitors)
• Control systemic hypertension
• All of these are most effective earlier, rather than later