Ca/Phosphate Homeostasis

Question 1

Where is most of the body’s calcium found?

Answer 1

99% of total body calcium found in mineralized osteoid of bone. 1% important in the cell (exchangeable pool)

Question 2

What is calcium needed for inside the cell?

Answer 2

Needed for muscle contraction, gland secretion, peristalsis, complement activation, and enamel formation.

Question 3

How much calcium intake daily?

Answer 3

1000 mg/d.

Question 4

How is calcium excreted?

Answer 4

700 mg/d fecal300 mg/d urineso balance is 0 in a healthy adult. In children, it is positive and in elderly it is negative

Question 5

Normal serum Ca levels?

Answer 5

8.7-10.2 mg/dl

Question 6

Normal ionized Ca component levels?

Answer 6

4.8-5.2 mg/dl

Question 7

Of the 1% of non-bone retained calcium, the majority is intracellular. How does the extracellular Ca+ exist?

Answer 7

roughly half is protein bound (and hence inactive) and ~half is in the free form (hence physiologically capable of involvement in processes). Well, a small part of the free form is also complexed to proteins but a major part is in the ionized free form and this is the component that is active.

Question 8

How does calcium enter enterocytes from the intestinal lumen?

Answer 8

TRPV6 channel through the brush border membrane along a favorable electrochemical gradient.

Question 9

How is Ca released from the BL side of the enterocyte?

Answer 9

Pumped out of the cell at the BL side against a steep electrochemical gradient by the Ca2+-ATPase.

Question 10

What happens when there is a major elevation of intracytoplasmic Ca2+ in the enterocyte?

Answer 10

Ca2+ leaves the cell using a Na+-Ca2+ exchanger instead on the BL.

Question 11

What else controls Ca efflux (and influx to some extent)?

Answer 11

Calcitriol, which binds the vitamin D receptor (VDR) which promotes absorption

Question 12

The late part of the distal convoluted tubule (DCT) and connecting tubule (CNT) play an important role in fine tuning renal excretion of Ca2+ and represents the bulk of ACTIVE reabsorption of Ca2+. How?

Answer 12

The epithelial Ca2+ channel (TRPV5) is primarily expressed apically in these segments and functions with calbindin- D28K (28K) on the apical surface and Na+/Ca2+ exchanger (NCX1), and the plasma membrane ATPase (PMCA1b) on the BL55% of Ca2+ reabsorbed in the PT-passive25% in the Thick ALH-mainly passive

Question 13

Describe the absorption of Ca2+ in the distal segments

Answer 13

Upon entry via TRPV5, Ca2+ is buffered by 28K and diffuses to the basolateral membrane where it is released and extruded by a concerted action of NCX1 and PMCA1b.

Question 14

What else does the BL membrane express?

Answer 14

In addition, the BL membrane exposes a parathyroid hormone receptor (PTHR) and the Na+/K+-ATPase consisting of the α-, β-, and γ-subunit.

Question 15

What does PTHR do?

Answer 15

PTHR activation by PTH stimulates TRPV5 activity, and entered Ca2+ can subsequently control the expression level of the Ca2+ transporters.

Question 16

What is BK2? Function?

Answer 16

At the apical membrane, a bradykinin receptor (BK2) is activated by urinary tissue kallikrein (TK) to activate TRPV5-mediated Ca2+ influx.

Question 17

How is Ca2+ regulated In the cell?

Answer 17

entered Ca2+ acts as a negative feedback on channel activity, and 28K plays a regulatory role by association with TRPV5 under low intracellular Ca2+ concentrations.

Question 18

What is Klotho? Function?

Answer 18

Extracellular urinary Klotho directly stimulates TRPV5 at the apical membrane by modification of the N-glycan, and intracellular Klotho enhances Na+/K+-ATPase surface expression that in turn activates NCX1-mediated Ca2+ efflux.

Question 19

What are calcium sensing-receptors (CaSRs)? Function?

Answer 19

Receptor on cells. Activation of the CaSR by calcium stimulates phospholipase C, leading to increased IP3, which mobilizes intracellular calcium and inhibits parathyroid hormone (PTH) synthesis. A decrease in serum calcium inhibits intracellular signaling, leading to increased PTH synthesis and secretion.

Question 20

How does the body respond to increased plasma Ca2+?

Answer 20

-activation of CaSR-leads to decreased PTH and increased fractional renal Ca excretion and calcitonin levels

Question 21

What does decreased PTH/increased calcitonin lead to?

Answer 21

decreased mobilization of Ca from skeleton and soft tissue and decreased renal 25-hydroxylation of vitamin D precursor

Question 22

What is the main function of vitamin D?

Answer 22

Ca intestinal absorption

Question 23

T or F. Serum Ca decrease slowly with age from infancy

Answer 23

T.

Question 24

What is the distribution of phosphorus in the body?

Answer 24

-85% bone-14% soft tissue-1% ECFtotal 700g

Question 25

Where is intracellular phosphorus stored?

Answer 25

in cell membrane phospholipids mainly

Question 26

Uses of phosphorus in the cell?

Answer 26

-mediator of Pi transfer (ATP/ADP, etc.)-DNA/RNA backbone linkage- Ionized inorganic phosphate also serves as a buffer to maintain the proper pH of body fluids.

Question 27

What is a very important use of phosphorus in RBCs?

Answer 27

The presence of 2,3-diphosphoglycerate in red blood cells facilitates the release of oxygen from oxyhemoglobin into body tissues.

Question 28

Daily intake of phosphorus

Answer 28

800-1500 mg

Question 29

How well is phosphorus absorbed?

Answer 29

At intake levels below 10 mg/kg/day, 80% to 90% is absorbed, while at intake levels above 10 mg/kg/day, only about 70% is absorbed via a Na-Pi transporter (we don’t know what the BL transporter is).There are also paracellular routes so intake cannot be fully stopped with drugs or disease

Question 30

Where in the GI does phosphorus uptake occur?

Answer 30

Absorption occurs throughout the intestinal tract, but primarily in the jejunum. Again, A variable amount of dietary phosphorus (10% to 30% of the ingested amount) is excreted through the GI tract.Keep in mind that it is the same transporter that is responsible for kidney reabsorption as is used in GI absorption

Question 31

What is the usual phosphorus urinary excretion in percentage of filtered load?

Answer 31

As blood is filtered through the renal glomerulus, 85% to 95% of phosphorus is partially resorbed at the PT and is not further reabsorbed until the distal tubule. The usual net load of phosphorus excreted is 5% to 15% of the filtered load. Not any in the ascending limbs

Question 32

T or F. Hyperphosphatemia is rare

Answer 32

T. Usually won’t occur until the GFR declines to less than 25 mL/min in patients with chronic renal insufficiency,

Question 33

Normal phosphorus levels?

Answer 33

2.5-4.5 mg/dl above GFR of 25 ml/min

Question 34

Normal excretion routes of phosphorus

Answer 34

assume 1400g daily intake900g urine500g fecal

Question 35

How is phosphate absorbed into enterocytes?

Answer 35

Phosphate enters the enterocyte (influx) through the brush border membrane by the Na+-Pi cotransport system, with a stoichiometry of 2:1, operating against an electrochemical gradient.

Question 36

How does Phosphate exit at the basolateral side?

Answer 36

possibly occurs by passive diffusion or (more probably) by anion exchange.

Question 37

Renal handling of phosphate

Answer 37

Tubular reabsorption of phosphate is saturableWith GFR>40 ml/min, TmP varies proportionately with GFR (TmP/GFR constant)With GFR less than 40, the kidneys cannot remove enough phosphate and hyperphosphatemia ensues

Question 38

How do we get vitamin D?

Answer 38

diet and sun (pro hormone in these forms)

Question 39

Metabolism of vitamin D.

Answer 39

Cholesterol is converted to 7-dehydrocholesterol which is converted to vitamin D3 via sunlight and diet gives vitamin D2 from plants and yeasts and vitamin D3 from fatty fishBoth Vitamin D2 and D3 bind to vitamin D binding protein (VDBP) and circulate to the liver.

Question 40

What happens once the vitamin D3 and D2 complexes reach the liver?

Answer 40

In the liver, vitamin D is hydroxylated by liver 25-hydroxylase (CYP27A1) to 25(OH)D, commonly referred to as calcidiol.

Question 41

What happens to calcidiol?

Answer 41

Calcidiol is then further metabolized to calcitriol by the tissue 1α-hydroxylase enzyme (CYP27B1) in the PT of the kidney. The active metabolite 1,25(OH)2D3 (calcitriol) acts principally on the target organs of intestine, the parathyroid gland, osteoclast precursors, and the kidney. OR it can be converted to 24,25(OH)2D which a very mildly active form of vitamin D (not common)

Question 42

Can activated vitamin D3 be inactivated/neutralized?

Answer 42

Yes, Calcitriol is metabolized to the inert 1,24,25(OH)3D through the action of the 24,25-hydroxylase enzyme (CYP24). Calcidiol is similarly hydroxylated to 24,25(OH)2D.

Question 43

What receptors in the PT tubular cell initiates endocytosis of DBP/25-OH-D3 complex?

Answer 43

megalin and cubulin. And then CYP27B1 acts This is found in target cells (and the kidneys) that are capable of activating caltriciol from the inactive form

Question 44

What happens to activated calcitriol?

Answer 44

It circulates bound to DBP. 1,25(OH)2D3 is then taken up by target cells and targeted to intracellular D-binding proteins (IDBP) to mitochondrial 24-hydroxylase or to the VDR.

Question 45

What does the 1,25(OH)2D3-VDR complex do?

Answer 45

It heterodimerizes with the retinoic acid receptor (RXR) and binds to specific sequences in the promoter regions of the target gene. The DNA bound heterodimer attracts components of the RNA polymerase II complex and nuclear transcription regulators.

Question 46

What is the initial PTH precursor product of the parathyroid?

Answer 46

A 84-aa protein that gets cleaved into N-terminal, C-terminal, and mid-region fragments

Question 47

What do first-generation PTH assays detect?

Answer 47

Full-length PTH (1-84) in addition to PTH fragments. These assays include radioimmunoassays (RIAs) that use antisera specific to the amino-terminal (N-RIA), middle (MID-RIA), or carboxyl-terminal (C-RIA) regions of PTH.

Question 48

What do second generation “intact PTH” assays detect?

Answer 48

full-length PTH (1-84) and non–(1-84) PTH fragments.

Question 49

What do third generation “intact PTH” assays detect?

Answer 49

Third-generation PTH assays (biointact PTH) detect only full length PTH (1-84).

Question 50

What does PTH bind to?

Answer 50

the PTH1R (GPCR)- increases cAMP, PKA, and then PKC to increase intracellular calcium (widely expressed in several tissues including the kidneys)

Question 51

Where is PTH1R found?

Answer 51

many tissues including the kidney and osteoblasts

Question 52

How does PTH regulate serum Ca levels?

Answer 52

Increased Ca2+ binds to the CaSR and causes IP3 to release SR calcium to decrease PTH. If Ca is low, this is blocked and PTH acts to increase bone resorption, increase renal calcium reabsorption and decrease Pi reabsorption, and up regulate 1a hydroxylase in the kidney, thereby increasing gastrointestinal calcium and Pi absorption.

Question 53

FGF (Fibroblast growth factor) exerts its effect in what fashion?

Answer 53

paracrine via binding to one of four distinct FGF receptor tyrosine kinase gene products (Fgfr1 to Fgfr4)

Question 54

What does FGF binding to its receptors require?

Answer 54

heparin

Question 55

Are any FGFs heparin independent? Why?

Answer 55

The FGF19 subfamily members (consisting of FGF19, FGF21, and FGF23) are heparin independent, resulting from unique structural features permitting them to circulate and act as endocrine factors:FGF19: energy and bile acid homeostasis;FGF21: glucose and lipid metabolism;FGF23: phosphate and vitamin D homeostasis

Question 56

Where is FGF23 found in the genome?

Answer 56

12p13

Question 57

What is the function of FGF23?

Answer 57

-Phosphaturic-Suppressor of 1-alpha hydroxylase in the kidney-Reduced renal phosphate reabsorption-Prevents soft tissue calcification

Question 58

Where is FGF23 mostly expressed?

Answer 58

Predominately expressed in osteocytes, but also ventrolateral thalamic nucleus, central venous sinusoids and thymus.

Question 59

What is an important cofactor for FGF23 action? Function?

Answer 59

Klotho - single pass TM protein necessary for FGF23-medicated receptor activation (stimulated by high calcitriol levels)decreases Pi PT reabsorption and 1a hydroxylase activity

Question 60

What is the difference between intermittent and constant production of PTH?

Answer 60

intermittent PTH release promotes serum Ca+ increase but constant release can have a counter effect

Question 61

What are the parts of bone?

Answer 61

-crystaline part-amorphous part-water (30%)the crystalline part is responsible for the exchangeable pool in the body

Question 62

When the amount of Ca2+ in the GI lumen is very high OR there is very low blood Ca2+ (aka there is a large gradient), what happens?

Answer 62

Paracellular absorption dominates (cant be saturated) over TRPV6. Because you want to absorb everything you can

Question 63

How do the kidney react to large increases in serum Pi? can they reabsorb it all?

Answer 63

No, tubular reabsorption of phosphate is saturableWhen GFR>40 ml/min, the amount reabsorbed is proportional that amount being taken in from the GI (i.e. the more taken up, the more excreted). When GFR is less than 40, more phosphate is reabsorbed and hyperphosphatemia ensues

Question 64

What are the regulators of renal phosphate handling?

Answer 64

-PTH-Dopamine-Phosphatonins (FGF-23, FGF-7)

Question 65

FGF-23 Function

Answer 65

Secreted by osteocytes in response to high phosphorus/ vitamin D3 signals. Binds to the heterodimer of FGF receptor and Klotho and the binding causes reduction of the NaPi cotransporter on the lumenal surface of the PT and down regulates 1a hydroxylase to reduce serum Pi levels Cleaved by furins when phosphate levels are normal to inactivate it.

Question 66

What cells can block vitamin D production?

Answer 66

melanocytes in skin

Question 67

T or F. While the kidneys are responsible for the vast (~90%) of vitamin D activation, there are target cells in the body that are capable of producing their own

Answer 67

T.

Question 68

What are some things that decrease PTH secretion?

Answer 68

-calcium via CaSR-calcitriol-FGF23 (direct inhibition of PTH mRNA expression)

Question 69

What are some things that increase PTH secretion?

Answer 69

-high phosphorus (pathologic in chronic kidney disease)-low calcium-FGF23 (decreased calcitriol synthesis)

Question 70

What are the effects of PTH (from low Ca2+)?

Answer 70

-increased 1a hydroxylase activity to increase calcitriol which increases GI Ca and PO4 absorption-increased bone turnover to increase serum Ca and PO4-increased renal Ca reabsorption and decreased PO4 reabsorptionSO the end game is increased Ca and NORMAL/slight decrease in PO4*

Question 71

What are the effects of low vitamin D?

Answer 71

-low vitamin 25(OH) D3 leads to low Ca2+ levels leading to increased PTH secretion and thus, dropping of phosphorus from the kidneyNote that the high levels of PTH can stimulate kidney 1a hydroxylase to make calcitriol from the low amounts of dicitriol as a compensatory mechanismTHIS CHANGES IN CKD

Question 72

What stimulates production of FGF23?

Answer 72

1,25(OH)2D, possible PTH(could be cause or effect), bone metabolism

Question 73

Adverse effects of FGF23?

Answer 73

-inflammation-vascular disease -increased RAAS-metabolic disorders via KLOTHO downregulation

Question 74

What does FGF23 do to KLOTHOS?

Answer 74

down regulates it through negative feedback

Question 75

What happens to FGF23 levels in CKD?

Answer 75

increased as phosphorus levels rise dramatically

Question 76

How does PTH increase bone turnover?

Answer 76

It binds to a receptor on osteoBLASTS to increase RANK and downregulate its inhibitor osteoproteregin. RANK then binds to RANKL to promote osteoclast formation