SM 204a/206a - CKD, CKD Clinical Flashcards
What is the mechanism of SGLT2 inhibitors?
Where do they act?
Which patients will benefit most from them?
SGLT2 inhibitors block Na+ and glucose absorption in the proximal tubule
This increases solute delivery to the macula densa
- -> Downregulation of RAAS
- -> Less Angiotensin II
- -> Less efferent arteriolar vasoconstriction
- -> Prevents intra-glomerular hypertension
- -> Decreased Na+ uptake along the rest of the tubule
- -> Decreased filtration
What are the acute (emergent) indications for starting dialysis?
AEIOU
- Acidosis
- Electrolytes (Hyperkalemia)
- Ingestions (Lithium, ASA)
- Overload (Volume overload)
- Uremia
- Nutrition (in pediatrics)
Usually dialysis is not started unless the patient is in distress/discomfort/generally is not doing well
Why do we get increased filtration in early-stage diabetic renal disease?
Diabetes
- -> Increased glucose load
- -> More SGLT2 channels = increased Na+ and glucose absorption in the proximal tubule
- -> less Na+ delivery to macula densa
- -> less Adenosine released
- -> Afferent vasodilation
- Macula densa mediates increased filtration
- -> Intraglomerular hypertension, increased filtration
SGLT2 inhibitors prevent afferent vasodilation and efferent vasoconstriction, thus reducing hyperfiltration and reducing intraglomerular hypertension
Why are patients with CKD at increased risk of free iron deficiency?
CKD = buildup of hepcidin
Hepcidin inhibits ferroportin, a protein necessary for iron reabsorption and recycling
CKD -> Hepcidin -> Decreased free iron
(Ferroportin is the channel through which iron is released from enterocytes and macrophages)
