AKI, CKD, Dialysis Flashcards

Question 1

Q

Features of rhabdomyolysis

Answer

A

Syndrome of muscle necrosis and release of intracellular muscle contents into circulation
Reddish brown urine due to myoglobinuria in half of cases
High CK, hyperkalaemia, hypocalcaemia, hyperphosphatemia, HAGMA

Question 2

Q

Post-obstructive polyuria leads to impairment in:

Answer

A

UO > 200ml/hr for 2 hours or >3L/day

Impairment in:

urine concentrating ability
sodium reabsorption
urinary acidification
potassium secretion

Question 3

Q

Acute Interstitial Nephritis

Answer

A

Drug exposure accounts for > 70% of AIN
Development of drug-induced AIN is not dose dependent and a recurrence/exacerbation of AIN can occur with second exposure to the same or related drug
Triad of rash, fever, eosinophilia
Can also cause eosinophiluria

Question 4

Q

How much protein should be eaten in patients with CKD to prevent progression

Answer

A

Reduced to 0.8g/kg/day

Question 5

Q

Top 3 causes of CKD

Answer

A

Diabetes
Glomerulonephritis
HTN

Question 6

Q

What is “fixable” and “unfixable” with dialysis

Answer

A

Fixable:
• Salt and water balance - fluid overload
• Clearance of “uraemic toxins” - uraemia
• Potassium homeostasis - hyperkalaemia
• Acid-base balance - metabolic acidosis

Unfixable
• Erythropoietin production - anaemia
• Vitamin D synthesis and phosphate - secondary hyperparathyroidism

Question 7

Q

Effect of CKD on other organ systems

Answer

A

Cardiovascular disease
Hyperparathyroidism
Uremic pruritus
Malnutrition
Uremic neuropathy
Sexual dysfunction: Reversible factors (testosterone, prolactin, oestrogen), sildenafil, optimise dialysis if needed

Question 8

Q

Definition of CKD

Stages of CKD

Answer

A

DEFINITION
- eGFR < 60 present for 3 MONTHS (with or without other evidence of kidney damage)
OR
Presence of the following >3 months (irrespective of GFR) 
- Albuminuria
- Glomerular haematuria
- Structural abnormality (on imaging) 
- Pathological abnormality ( on biopsy)

Stage 1: GFR >90 
Stage 2: GFR 60-89 
Stage 3a: GFR 45-59 
Stage 3b:  GFR 30-44
Stage 4: GFR 15-29 
Stage 5: <15 or dialysis

Stage 3A CKD with macroalbuminuria is normally due to diabetic kidney disease

Normal Urine ACR
- Male < 2.5, Female < 3.5

Microalbuminuria
Male Urine ACR: 2.5-25mg/mol
Female Urine ACR: 3.5-35mg/mmol

Macroalbuminuria
Urine ACR Male > 25mg/mmol
Urine ACR Female > 35mg/mmol

Question 9

Q

eGFR

Answer

A

Assumes steady state of creatinine generation and excretion
Useful for monitoring patients in CKD
Not appropriate in:
AKD/AKI
Children
Pregnancy
Extremes of body weight
Patients taking extra creatinine

Question 10

Q

What is used to calculate eGFR

Answer

A

CKD-EPI?
The CKD-EPI (Chronic Kidney Disease Epidemiology Collaboration) is currently used now

More accurate at higher eGFR
– Validated across more populations
– Better prediction of adverse clinical outcomes cf. MDRD

Question 11

Q

What is the most common cause of death in CKD and transplant

Answer

A

CKD: Withdrawal is the most common cause of death followed by cardiovascular events
Transplant: cancer and cardiovascular disease is the most common cause of death

Question 12

Q

CV disease and CKD

Answer

A

Cardiovascular disease
– Principal cause of death at all stages of CKD
– Left ventricular hypertrophy
– Myocardial fibrosis
– Accelerated vascular disease (non-atherosclerotic)
– Widened pulse pressure

Antihypertensive agents (beta-blockers, RAS blockers) effective
Lipid lowering agents not proven to be effective

Question 13

Q

CKD and anaemia

Answer

A

Common: less with ADPKD
Proportional to CKD

Multifactorial

Inflammation
Higher blood loss
Hyperparathyroidism
Dysfunctional iron access
Reduced EPO

Target Hb 110-120
Needs sufficient iron (T sats >20%, ferritin > 300)

Does not increase length life
Improves QOL
Reduces transfusions

Question 14

Q

Causes of EPO resistant anaemia

Answer

A

Iron deficiency (most common cause)
Intercurrent infection
Hyperparathyroidism
Primary bone marrow pathology
Folate/B12 deficiency
Pure red cell aplasia
Production of antibodies against EPO related to exogeneous treatment.
Less common with newer diluents.

Question 15

Q

Side effects of EPO

Answer

A

– Hypertension (commonest) - can be associated with
hypertensive encephalopathy
– Thrombosis of access
– Pure red cell aplasia

Adverse effects of higher Hb targets (death 45 – 48% increased risk, CVA, vascular access thrombosis) well
proven

Question 16

Q

Causes of iron deficiency in HD patients

Answer

A

Most patients on HD are not physically able to absorb enough orally absorbed iron to prevent iron deficiency
– Loss of blood during dialysis (10-30mL)
– Increased mucosal loss (anticoagulation during dialysis)
– Clotted circuit – 200-500mL blood
– Low haem iron diet
– Increased hepcidin (reduces GI duodenal iron absorption by binding ferroportin and sequestering iron in the macrophages)

Hepcidin is a key regulator of iron homeostasis and plays a role in the pathogenesis of anaemia of chronic disease. Its levels are increased in patients with chronic kidney disease (CKD) due to diminished renal clearance and an inflammatory state.

Question 17

Q

Iron management in HD

Answer

A

Target levels
– Ferritin > 300ug/mL
– Transferrin saturation > 20%

Intravenous iron required in majority
– Oral iron absorption poor and cannot replace average
daily iron loss
– Typically infused during HD treatment
– Maintenance protocols more effective than ‘reactive’ protocols
– Withhold during active infection

Question 18

Q

How much renal function is substituted by dialysis?

Question 19

Q

Which patients are excluded from peritoneal dialysis

Answer

A

Obese patients
Abdominal surgery
Poor vision
Unstable home environment
Not attentive to hygiene
Patients without any residual renal function
If anuric or passing urine <500ml/day then they need to be transitioned to dialysis
RESIDUAL RENAL FUNCTION is required for a patient to undergo peritoneal dialysis

Question 20

Q

PD vs HD

Answer

A

PD catheter inserted 2-3 weeks before starting PD
Patients need RESIDUAL RENAL FUNCTION for PD
HD: fistula created 2-3 months prior

When to start dialysis
- eGFR 5-10ml/min
- Uraemic symptoms eg: itch, cognitive dysfunction, fatigue, SOB, muscle cramps, N+V
- Fluid overload that cannot be treated with
diuretics/fluid and salt restriction
- Hyperkalaemia that cannot be managed with dietary vigilance and potassium binders
- Pericarditis, uraemic encephalopathy

AEIOU
Acidosis
Electrolytes
Ingestion of toxins
Overload 
Uremia

Question 21

Q

Haemodialysis access sites

Answer

A

AV fistula
AV grafts
Tunnelled dialysis catheters
Descending in order for greater infection risk and less reliable

Question 22

Q

Dialysis catheter related bacteremia and tx

Answer

A

• 40-80% gram positive
• S aureus CRB associated with 20-30% mortality
• ‘Around catheter’ contamination more common than ‘inside catheter’
• Higher in
– Patients with diabetes
– Non tunnelled lines
– Femoral>internal jugular>subclavian

• Always assume the catheter is source of infection in a febrile dialysis
patient until proven otherwise
• Cultures from catheter and peripheries
• Mandatory removal (send tip for culture) if
– Non tunnelled line
– Severe sepsis in tunnelled line
• Broad spectrum antibiotics
– Empiric vancomycin or linezolid if MRSA/ VRE colonised
– Include gram negative cover
– 14 days treatment for S aureus
• Evaluate for metastatic infection (endocarditis, osteomyelitis, epidural
abscess) if persistent fevers or bacteraemia

Question 23

Q

Which of the following statements regarding haemodialysis (HD) and peritoneal dialysis (PD) is correct?

a. Patients on PD suffer greater fluctuations in their fluid state than patients on HD
b. Both HD and PD lose their effectiveness with time
c. Low serum urea levels are a reliable indicator of effective therapy
d. Weight gain in the absence of fluid overload commonly occurs in patients on PD
e. HD has a proven advantage over PD in preservation of residual kidney function.

Answer

A

d. Weight gain in the absence of fluid overload commonly occurs in patients on PD

Question 24

Q

Which of the following is true regarding mortality in HD patients?
a. Similar to the general population when high quality HD has been given
b. Commonest cause of fatality is infection
c. Fatality in HD patients is highest after a longer interdialytic break
d. Cardiovascular mortality is explained by traditional CV risk factors
e. Statin therapy for hyperlipidaemia has an established role in high risk patients on HD

Answer

A

c. Fatality in HD patients is highest after a longer interdialytic break

Question 25

Q

In PD, how do solute and water move across the peritoneal membrane?

Answer

A

3 transport processes occurring at the same time
1. DIFFUSION – where substances of high
concentration move towards areas of low
concentration.

CONVECTION – the difference in osmolality leads to movement of water and associated solutes across the
membrane.
ABSORPTION – the lymphatics constantly absorbs water and solutes.

Peritoneal Clearance is the net result of diffusion + convection – absorption.

Question 26

Q

Diffusion in PD

Answer

A

This is critical for removal of uraemic toxins in peritoneal dialysis.

Relies on –
• Concentration gradient
• Effective peritoneal surface area
• Intrinsic peritoneal membrane resistance
• Molecular weight of the solute concerned

Question 27

Q

(A) How can peritoneal clearance by increased?

(B) How can fluid removal be increased by?

Answer

A

(A) Peritoneal CLEARANCE can be increased by:
1. Maximising time on PD

Maximising concentration gradient
• Increasing number of exchanges
• Increasing dwell volumes
Maximising effective peritoneal surface area
• Increasing dwell volumes
Maximising peritoneal fluid removal

(B) FLUID REMOVAL can be increased by:
1. Maximising the osmotic gradient
• Higher glucose concentration
• Increase number of exchanges

Use an osmotic agent that is not absorbed well
Increase urine output

Increase in % of bags = increase amount of fluid removed
Different Bags: 1.5%, 2.5%, 4.25%, 7.5% (isodextrin)
Increase in fill volume/number of cycles = increase solute clearance (eg: urea, K+)

Question 28

Q

What is the peritoneal equilibration test?

Answer

A

Gives us an idea of the transport characteristics of an individual’s peritoneal membrane
Assessed by using equilibration ratios between dialysate and plasma for urea (D/P urea), creatinine (D/P creatinine)
By waiting for equilibration, this test measures the combined effect of diffusion and convection.
UF volumes are inversely proportional to peritoneal transport characteristics for solutes
High transporters rapidly absorb the osmotic agent into peritoneal capillaries, diminishing stimulus for ultrafiltration within a few hours of dwell, leading to reabsorption of fluid through rest of the dwell
Low transporters have good ultrafiltration, because the osmotic gradient is maintained throughout the entire dwell

High Transporters:
- Benefit from APD modalities that use shorter dwell times (so they need more cycles for better solute clearance)
- Excellent solute clearance
- Poor ultrafiltrate
· High Transporters: require more cycles for better solute clearance, normally diabetics are high transporters

Low Transporter

Benefit from longer dwell modalities such as CAPD
Inadequate solute clearance
Excellent ultrafiltration
Patients with a so-called high transport status of the peritoneal membrane (i.e. a more permeable peritoneal membrane), characterized by a high dialysate to plasma (D/P) ratio of creatinine, have a low UF volume due to rapid dissipation of glucose from the PD fluid to the capillaries.

· Low Transporters: it would be ideal to start as a low transporter as most PD patients progress to being high transporters
○ The ideal would be to be a low transporter and non-diabetic
· Low Transporter –> High Transporter –> Membrane Failure
○ Membrane Failure: when dwell time of 4 hours, 4.25% bags, UF <400mL
When there is membrane failure, the patient will need to be transitioned from PD to HD

Question 29

Q

What are high transporter states

Answer

A

Inherent high transporter
Peritonitis: transient and reversible
Acquired on long term PD, esp in patients with a greater cumulative dextrose load

Question 30

Q

Types of PD

Answer

A

2 main Types: APD (automated peritoneal dialysis) vs CAPD (continuous ambulatory peritoneal dialysis)

○ APD (automated): using a cycler, done at night, frees up the morning/afternoon, overnight using machine

○ CAPD (continous ambulatory): manual, done by the patient - 3 manual bags in the morning + afternoon and isodextrin bag at night 4-5 bags/day every day
§ Patients who are on CAPD are normally low transporters

Question 31

Q

Benefits of 7.5% icodextrin

Answer

A

Relatively inert high molecular weight polymaltose
glucose polymer
Less permeable than dextrose - ultrafiltration occurs for
a longer period of time.
Equivalent UF volume as a 4.25% dextrose
Best used in a long dwell
Reduced carbohydrate load
Potential advantage of reducing the long term metabolic complications associated with hypertonic dextrose

No impact on
– Residual renal function
– Urine output
– Incidence of peritonitis
– Peritoneal creatinine clearance
– Technique failure
– Patient survival

Icodextrin can lead to:
- Over estimation of Blood Glucose levels
with Glucometers based on glucose
dehydrogenase (Advantage, Acucheck)
- Under estimation of Serum amylase level
(false low)

Question 32

Q

Using low GDP (glucose degradation products) neutral pH solutions

Answer

A

Low GDP, neutral pH solutions on
other outcomes

• Preserved urine output
• Less inflow pain
• No effect on:
– Ultrafiltration
– Peritoneal clearances
– Peritonitis episodes
– Technique failure
– Mortality

Question 33

Q

Methods to preserve residual renal function with patients on PD

Answer

A

Use of ACEi/ARBs for treatment of hypertension
Low GDP, neutral pH PD solutions

Avoid
• Prolonged use of Aminoglycosides
• NSAIDS
• Contrast agents

GDP: glucose degradation products

Question 34

Q

What conditions favour PD vs HD

Answer

A

Favours PD

BP control
Lower EPO dose
Quality of life as able to do at home

Favours HD

CCF
Hypoalbuminaemia
Survival from critical illness in ICU

Question 35

Q

Indications for PD catheter removal

Answer

A

Indications for catheter removal include:
- refractory peritonitis (failure to respond to appropriate antibiotics within 5 days)
- relapsing peritonitis
- refractory exit-site and tunnel infection
- fungal peritonitis.
Also consider catheter removal if the patient is not responding to therapy, in infections caused by mycobacteria, or in polymicrobial infection with enteric pathogens.
If removed may require vascath for haemodialysis

Question 36

Q

Complications of PD

Answer

A

Infective

Peritonitis
Exit site infection
Tunnel Infection

Pressure related: intra-abdominal pressure lowest when supine, greatest while sitting

Hernias
Dialysate leaks: pericatheter, abdominal, genitalia, pleural

Non-infective
- Access Related:
Catheter obstruction
Omental entrapment
Tip migration can occur due a mass or constipation 
Cuff extrusion
- Ultrafiltration failure
- Technique failure

Question 37

Q

PD Peritonitis Features

Answer

A

Clinical features consistent with peritonitis: abdominal pain, cloudy dialysate
Dialysate WCC > 100, >50% polymorphs/neutrophils, positive gram stain

The most common pathogens are:

Coagulase-negative staphylococci (eg Staphylococcus epidermidis)
Staphylococcus aureus
enteric Gram-negative bacilli
Streptococcus and Enterococcus species.
Infection with fungi is uncommon

Microbiology:
• 50% Gram positives = SKIN
- coagulase negative staph, staph aureus, enterococcus, streptococcus
• 15% Gram negatives = GUT
• 20% Culture negative = Don’t Know
• 4% Polymicrobial infection = Laparotomy/Remove Tenckhoff
• multiple Gram negatives or Gram positives and Gram negatives
• <2% Fungal infection = Panic and remove Tenckhoff
• 13% exit site infection
• 3% peritoneal fluid leak
• 31% hospitalization i.e. most treated in the community

Tx:
- IP Gentamicin 80mg daily (added to 1 bag of dialysis fluid) if level <0.6 for 2 weeks [dwell time 6 hours]
- IP Cephazolin 1.5g daily (added to 1 bag of dialysis fluid) [dwell time 6 hours]
o Replace cephazolin with vancomycin if history of MRSA, systemic symptoms or immediate hypersensitivity to penicillins - IP Vancomycin 2g daily if level <20 for 2 weeks
- IP Heparin 1000 units to be given with IP antibiotics or IP heparin 500 units/L of PD fluid (ie: 1000 units in a 2L bag of PD fluid)
- Antifungal Cover: PO Nilstat 1mL QID - to cover for fungal infections
- Gram Negative/enterococcus: can add PO ciprofloxacin 250mg BD, enterococcus does not respond to cephalosporins
Gram Positive: can add PO keflex

Recurrent peritonitis can result in sclerosing peritonitis which is fatal

Question 38

Q

Differential diagnosis of cloudy effluent

Answer

A

Culture-positive infectious peritonitis
Infectious peritonitis with sterile cultures
Chemical peritonitis - Eosinophilia of the effluent
Hemoperitoneum
Malignancy (rare)
Chylous effluent (rare)
Specimen taken from “dry” abdomen

Question 39

Q

Risks for renal progression

Answer

A

Proteinuria
Hypertension

Proteinuria most important marker for progressive renal failure
• Reducing proteinuria key goal of renal preservation
• Hypertension reduction vital to delay CKD progression
• Aggressive BP targets i.e. 125/75 (<130/80) in patients with diabetic and nondiabetic
nephropathy with proteinuria.
• ACE-I or ARBs for proteinuric nephropathies, combination no longer
recommended.
• Tight glycaemic control essential in diabetics.
• Salt restriction and bicarbonate therapy appear beneficial
• All other renal protection methods e.g. protein restriction, statins not sufficient
evidence to ask questions about.

Question 40

Q

How doe proteinuria cause damage?

Answer

A

Damage via:
– Hyperfiltration
– Tubular toxicity from resorbing certain proteins
– Increased tubular work
– Mesangial toxicity

Proteinuria thought to be reduced by reducing intraglomerular pressure – hence ACEi

Question 41

Q

Risk factors of renal failure

Answer

A

GFR < 90 
Diabetes 
Age 
Hypertension 
Smoking 
BMI

Question 42

Q

Which risk factor best predicts development of renal failure?
A. Age
B. Smoking
C. Hypertension
D. Obesity
E. GFR<90

Answer

A

E. GFR<90

Question 43

Q

A 60-year-old man with a five-year history of type 2 diabetes presents
for a routine check-up. The most appropriate screening test for diabetic
nephropathy is:
A. serum creatinine level.
B. spot urine albumin concentration.
C. 24 hour urine protein excretion.
D. spot urine albumin/creatinine ratio.
E. 12 hour urinary albumin excretion rate

Answer

A

D. spot urine albumin/creatinine ratio.

Question 44

Q

CKD and Hypertension

Answer

A

Aim BP < 120
Non Pharm
- Salt restriction (<2g/day) or <90mmol Na/24 hour
- Exercise: 150min/week

Question 45

Q

67 y.o. diabetic has significant renal impairment with the following results:
Creatinine 180􀈝mol/L (eGFR 34ml/min)
Hb 105 gm/L (115 - 135 gm/L)
Proteinuria 0.38 gm/day (<0.12 gm/day)
Blood pressure 150/90 mmHg and HbA1c 7.5%
Which of these is likely to have the greatest impact on slowing the
progression of CKD?
A. Blood pressure reduction.
B. Tight glycaemic control.
C. Erythropoietin therapy.
D. Control of serum phosphate.
E. Low protein diet.

Answer

A

A. Blood pressure reduction.

Question 46

Q

65 y.o. woman presents with vague symptoms of fatigue. The following biochemistry is noted:
Potassium 5.5 mmol/L [3.5-5.5]
Urea 48 mmol/L [<6.5]
Creatinine 1010 􀈝mol/L [<120]
Calcium 2.1 mmol/L [2.1-2.5]
Phosphate 2.3 mmol/L [0.8-1.4]
BP 165/95 mmHg, no oedema.
Apart from the fatigue she is asymptomatic, although some scratch marks are noted.
She has 8.8 cm kidneys without obstruction.
PHx of cholecystectomy and perforated appendix.
What is the most appropriate next step?
A. Urgent haemodialysis.
B. Urgent peritoneal dialysis.
C. Elective haemodialysis.
D. Elective peritoneal dialysis.
E. Urgent continuous venovenous haemodiafiltration

Answer

A

C. Elective haemodialysis.

Question 47

Q

Indications for URGENT dialyis s

Answer

A

• Hyperkalaemia
• Fluid overload
• Uraemic:
- Pericarditis
- Pleuritis
- Encephalopathy
- Bleeding

• Relative indication
- Urea >60 (creatinine level irrelevant)

Question 48

Q

In a patient requiring urgent dialysis which of the following parameters
would favour continuous renal replacement therapy (CRRT) rather than
intermittent haemodialysis (IHD)?
A. Active bleeding.
B. Coagulopathy.
C. Hyperkalaemia.
D. Hypotension.
E. Hypoxia.

Answer

A

D. Hypotension.

Question 49

Q

Pros and Cons of HD

Answer

A

Pros
• Efficient solute removal, reasonable fluid removal
• Intermittent – escape

Cons
• Intermittent –fluctuation in solute and fluid removal, BP
• Requires good cardiac function - weak hearts might suffer on HD
• Access can be difficult, especially in diabetics
• Heparin exposure
• Blood exposure to artificial circuit
• Strict attention required to fluid and solute intake

Question 50

Q

Pros and Cons of PD

Answer

A

Pros
• Smooth removal of solute and fluid
• Cardiac friendly
• No heparin. No blood contact with artificial products.
• Quick to learn -independence

Cons
• Peritonitis and Exit site infection
• Inefficient – reliance on residual renal function (protect)
• Respiratory embarrassment
• Requires dexterity +vision

Question 51

Q

67 y.o. diabetic on PD presents with abdominal pain, low grade fever and cloudy
dialysate. She has mild generalised abdominal tenderness and guarding but does
not appear particularly unwell. She is started on intra-peritoneal cephalexin. The
next day, her dialysate culture grows:
Enterococci, E-coli and Klebsiella species.
The most appropriate management step is:
A. exploratory laparotomy.
B. add intraperitoneal Ampicillin.
C. removal of the Tenckhoff catheter.
D. intraperitoneal gentamicin.
E. change to intravenous antibiotics.

Answer

A

A. exploratory laparotomy.

This is because there is 3 enteric bugs and this may indicate a bowel perf somewhere

Question 52

Q

With regards to haemodialysis patients, survival is improved by?
A. Tight BP control
B. Tight weight control
C. Dialysis dose
D. Dialysis duration
E. Tight cholesterol control

Answer

A

D. Dialysis duration

Question 53

Q

Dialysis Adequacy

Answer

A

URR (urea removal ratio) = (pre-dialysis urea - post-dialysis urea)/ pre-dialysis urea
goal>70%

Kt/V
• where K’ is the dialyser clearance, ‘t’ is time, ‘V’ is the volume of body water
• Kt/V = clearance x time ÷a volume estimate of body water
• Kt/V thus represents the volume of body fluid completely cleared of urea -the
chosen marker - in a single dialysis

Question 54

Q

Complications of renal failure

Answer

A

Cardiovascular disease
Anaemia
Renal bone disease
Hypertension
Hyperlipidaemia

Question 55

Q

A 71-year-old woman with hypertension and a remote smoking history of 20 pack years is found to have abnormal kidney
function on a routine blood test. Her current medication is enalapril 10 mg daily and amlodipine 10 mg daily and her last blood
pressure was 138/86 mmHg.
Her results are as follows: Normal values
Serum creatinine 168 􀈝mol/L [49–90]
Estimated glomerular filtration rate (eGFR) 31 mL/min/1.73 m2 [90–130]
Sodium (Na) 138 mmol/L [134–145]
Potassium (K) 4.7 mmol/L [3.5–5.0]
Haemoglobin (Hb) 116 g/L [120–160]
Calcium (Ca) 2.45 mmol/L [2.20–2.55]
Phosphate (PO4) 1.3 mmolL [0.78–1.43]
Urine albumin:creatinine ratio (ACR) 11 mg/g [< 3.5]
In addition to monitoring kidney function, what additional strategy should be the focus of her management?
A. Dietary potassium restriction.
B. Modification of cardiovascular risk.
C. Planning for dialysis access.
D. Reduction of proteinuria.
E. Repletion of haematinics.

Answer

A

B. Modification of cardiovascular risk.

Question 56

Q

Role of statins in CKD

Answer

A

No clear benefits seen in dialysis patients
Calcific disease rather than lipid-rich plaques

Calcium & Phosphate
• Treat the phosphate for the vessels as well as the bones
• Major cause of death is vascular disease (44% - cardiac, another
11% vascular)
• This isn’t necessarily rupture of lipid-rich plaques, much of it is stenotic disease.

Question 57

Q

65-y.o. on HD for 9/12, is on EPO 4,000u 2x/week. Previously Hb had been stable
(105 – 115 gm/L).
She now presents with a Hb of 89 gm/L. There have been no changes to her EPO
dose or other medications.
MCV 84 fL [78-98]
Serum iron 13 􀈝mol/l [13-35]
Iron saturation 18% [15-46]
Serum ferritin 630 􀈝g/l [20-300]
Retic count 30 x 109/L [12-100]
Which is the most likely cause for her EPO resistance?
A. Inflammation.
B. Pure red cell aplasia.
C. Vitamin B12 deficiency.
D. Iron deficiency.
E. Hyperparathyroidism.

Answer

A

A. Inflammation due to ferritin

Question 58

Q

Cardiovascular disease is the major cause of death in dialysis patients. Elevation
of which of the following clinical parameters carries the highest mortality risk?
A. Serum phosphate.
B. Serum cholesterol.
C. Serum homocysteine.
D. Serum parathyroid hormone.
E. Blood pressure.

Answer

A

A. Serum phosphate.

High phosphate = higher mortality

Question 59

Q

Treatment of hyperphosphatemia in CKD

Answer

A

Reduce PO4 - dialysis, binders

• Binders:

calcium based –caltrate, cal-sup
Magnesium -mylanta
Aluminium -alutabs
Non-Calcium based = lanthanum (Fosrenol), sevalamer (Renagel)

Prevent hyperparathyroidism as high PTH causes increased urinary phosphate excretion

Replace vitamin D (1,25) to maintain normal calcium levels
Use vitamin D as suppressive therapy
If non-responsive consider calcimimetics (eg: cinacalcet) or PTHectomy (PTH>100)

• Avoid calcium based PO4 binders if calcium is high

Question 60

Q

Which of the following is most likely to increase serum phosphate in chronic renal
failure?
A. Calcium trisilicate.
B. Calcitriol.
C. Cinacalcet.
D. Calcitonin.
E. Alendronate.

Answer

A

B. Calcitriol

Vit D increase Ca and Po4
PTH just cares about Ca, increases Ca and decreases PO4

Vitamin D is about making bone

Increased gut absorption of Ca nad Phosphate
Reduced urinary losses of Ca and Phosphate

PTH is about maintaining serum Ca

Reduced urinary loss of Ca
Increased urinary loss of Phosphate

Question 61

Q

Cinalcacet

Answer

A

Bind calcium sensing receptor and increase sensitivity to calcium (Cinacalcet/ Sensipar) useful for secondary hyperparathyroidism
Reduced parathyroidectomy rate
No evidence of improved mortality
with their use
No longer on PBS for CKDMBD

Question 62

Q

Renal bone disease in CKD

Answer

A

Hyperparathyroidism -osteitis fibrosa/ osteomalacia
Low vitamin D (active form) –decreased bone mineralisation (osteopaenia)
Adynamic bone disease/aluminium deposition – increased fracture risk
Don’t say osteoporosis in written or long case

Question 63

Q

Features of calciphylaxis

Answer

A

• Subepidermal calcific obstruction of
small vessels
• May be precipitated by hypotension
• Central type associated with mortality
>50%
• Treatment difficult, includes hyperbaric
oxygen and reductions in calcium and
phosphate.
• Sodium thiosulphate (also a role as an antidote to cyanide poisoning, a nephroprotective agent and an antifungal drug)

Question 64

Q

Treatment of vascular calcification in CKD

Answer

A

• Vascular calcification is a big issue (beware questions on this) need to reduce
phosphate, PTH, calcium and CaxPO4 product
• most important REDUCE PHOSPHATE

Answer 64

A

Marker of mortality

Answer 65

A

Acute Kidney Injury: defined as a sudden loss of renal failure with consecutive rise in creatinine and blood urea nitrogen.
As defined by the International Society of Nephrology (KDIGO)
- Urine Volume < 0.5mL/kg/hour for 6 consecutive hours (<400ml/day or <20ml/hr) OR
- Increase in serum creatinine by >26.5umol/L in 48 hours OR
- Increase in serum creatinine by 1.5x baseline within 7 days

Answer 66

A

Weight <60 kg, age >80 years, serum creatinine >133 micromol/L—use a lower dose for AF in the presence of at least 2 of these factors.

Answer 67

A

Pre-Renal (renal hypoperfusion, 70%): consider shock, dehydration, vomiting, diarrhoea, cardiorenal syndrome, renal artery thrombus

True volume depletion –gastrointestinal loss (vomiting, diarrhoea, bleeding);
renal losses (diuretics, glucose osmotic diuresis); skin or respiratory losses
(insensible losses, sweat, burns); third space sequestration (crush injury or
skeletal fracture);
Hypotension – Severely decreased blood pressure can result from shock
(hypovolemic, myocardial, or septic)
Drugs – that decrease afferent (pre glomerular dilatation) i.e. NSAIDs, Calcineurin inhibitors (cyclosporine, tacrolimus) OR decrease efferent (post glomerular) arteriolar constriction i.e. ACE-inhibitors or angiotensin II blockers OR cause volume depletion i.e. diuretics
Oedematous states- decreased cardiac output in CCF and splanchnic venous
pooling and systemic vasodilation in cirrhosis causing reduced renal
perfusion(Hepatorenal syndrome)

Answer 68

A

Glomerular: Glomerulonephritis, thrombotic microangiopathy, vasculitis
Can have dysmorphic RBC and RBC casts
Tubulo -interstitial: Acute tubular necrosis (ATN) and Acute interstitial nephritis (AIN)

Answer 69

A

ATN- defined by histologic changes- necrosis of the tubular epithelium
and occlusion of the tubular lumen by casts and cell debris; 3 major
causes of ATN are:
- Renal ischemia: All causes of severe prerenal AKI particularly hypotension, shock and surgery

Sepsis: Usually associated with hypotension
Nephrotoxins- aminoglycosides, vancomycin, cisplatin, radiocontrast
material, cidofovir

Often cause BLAND URINE

Usually caused by ischaemia - extension from pre-renal, usually secondary to pre-renal causes with continuing intravascular depletion, hypotension and renal ischaemia
Prolonged hypovolemia/shock
Thromboembolism
Thrombotic microangiopathy

Nephrotoxins (radiocontrast, myoglobin, radiation, drugs)
- Endotoxins: myoglobin (eg: rhabdomyolysis), casts (eg: MM)
- Exotoxin: aminoglycosides, IV contrast, chemotherapies
- Contrast induced nephropathy - to reduce the risk of this, should pre and post hydrate with isotonic NaCl
- Medications: aminoglycosides, cisplatin, anti Hep C medications (affecting proximal tubules)
- Pigment Nephropathy
□ Myoglobinuria due to rhabdomyolysis
□ Haemoglobinuria associated with haemolysis
- Acute uric acid nephropathy

Medications: aminoglycosides, amphotericin B, IV contrast, chemotherapy
Poisons: ethylene glycol, mercury, carbon tetrachloride
Endogenous Substances: myoglobin, Bence Jones Protein, amyloid
Occurs rapidly in 24 hours

Clinical Course

Injury can predate changes to sCr
sCr usually plateaus once parenchymal injury established
Oliguria is a predictor of the need for KRT
Polyuria usually heralds renal recovery and occurs prior to improvements in sCr
Severe ATN can result in cortical necrosis

Answer 70

A

Caused by inflammatory infiltrate in the renal interstitium (glomeruli normal)

Causes
- Drugs (NSAIDs, penicillins, cephalosporins, ciprofloxacin, PPIs,
diuretics etc.) : 70 to 75%
- Infections : Streptococcus, legionella, CMV 4-10%
-Tubulointerstitial nephritis and uveitis (TINU) syndrome –5-10%
- Systemic diseases: Sarcoidosis, Sjögren’s syndrome, SLE and others: 10-20%

Presentation

May present from few days to months after drug exposure
Triad of rash, fever, eosinophilia
Can also cause eosinophiluria
White cell casts

Tx:
- Discontinuation of the potential causative agent is a mainstay of therapy
- 2-3 months course of prednisolone in those whose creatinine does not improve
within 7 days of stopping offending drugs

Answer 71

A

· Post-Renal (5%):
- PUJ
- Ureters: stones, cancer
- Bladder + Prostate: BPH, carcinoma of cervix, stones, cancer, neurogenic bladder
- Urethra: stones/cancer/benign prostatic hyperplasia/catheter blockage
- + Neurological
For post renal: should do renal US/CTKUB/bladder scan post void

Answer 72

A

Renal vasculitis or AIN

Answer 73

A

Urine sodium concentration:
- Urine Na concentration is low in prerenal
disease (less than 20 mEq/L) in an attempt to conserve Na
- Urine Na concentration is high in ATN
(more than 40 to 50 mEq/L) due to impaired tubular function induced by the tubular injury

Fractional excretion of sodium: Better indicator than above

FENa < 1% usually indicates prerenal AKI (indicative of sodium retention)
FENa > 2% indicates (not always) ATN (damaged tubules unable to reabsorb Na)

Answer 74

A

Hypercalcemia in myeloma causing AKI needs aggressive hydration
Cast nephropathy in myeloma causing AKI needs urgent steroids/anti myeloma treatment

Answer 75

A

- Usually reversible, consequences
obviously dependent on intercurrent
patient issues
- Definition: >25% increase in SCr in 48
hours without another identifiable cause

RF:

Pre-existing CKD or low renal perfusion (e.g. CCF, dehydration)
Age >70
Multiple myeloma
Diabetes
Volume and type of contrast media used
Inpatients (?independent risk factor)
Drugs like NSAIDs, ACE inhibitors and ARBs

Pathogenesis: both renal medullary hypoxia due to vasoconstriction and direct tubular injury lead to ATN

Unlike other types of ATN, rapid recovery
AKI usually within 24 - 48 hours of contrast administration and improvement within three to seven days

Treatment
- avoid nephrotoxins, pre and post IV hydration with 0.9% saline or NaHCO3

Answer 76

A

Cholesterol crystal embolization to the kidneys
Usually after coronary angiography (commonest cause), renal angiography or
cardiovascular surgery
AKI several weeks later (sometimes within 1-2 weeks)
Urine bland, can have microscopic haematuria and minimal protein
Cyanosis or discrete gangrenous lesions in the toes with intact peripheral pulses (blue toes), livedo reticularis and focal neurologic deficits, orange plaques in the retinal arterioles (Hollenhorst plaques)
May be accompanied by-eosinophilia, eosinophiluria, and hypocomplementemia

Tx:
Supportive therapy and secondary prevention of CV disease with aggressive
lipid lowering therapy

Answer 77

A

Aminoglycosides freely filtered across glomerulus and partially taken up by
the proximal tubular cells
Gentamicin levels inside PTC cells 100 to 1000 times serum levels……toxic to
the cells
Non-oliguric AKI usually occurs 5 to 10 days after treatment with gentamicin
Involvement of the distal tubular cells may lead to hypokalemia and
hypomagnesemia

Answer 78

A

Myoglobin and haemoglobin are filtered by the glomerulus into the urinary space
and degraded releasing heme
Dipstick-positive haematuria in the absence of any RBC by microscopy may be the first clue along with pigmented granular casts

Heme can lead to AKI by three processes:

Tubular obstruction, possibly in association with uric acid
Direct proximal tubular cell injury
Vasoconstriction leading to medullary hypoxia
Also in rhabdomyolysis sequestration of large amounts of fluid in the injured
muscle can cause hypovolemia and pre renal AKI
Treatment consists of fluid replacement and at times alkaline diuresis with
intravenous bicarbonate to reduce chances of tubular obstruction

Answer 79

A

HRS is a reversible and functional renal failure that occurs in patients with
acute or chronic liver disease and portal hypertension

Diagnostic Criteria

Diagnosis of cirrhosis and ascites
Diagnosis of AKI
No response after 2 consecutive days of diuretic withdrawal and volume expansion
Absence of shock
No current or recent treatment with nephrotoxic drugs
No macroscopic signs of structural kidney injury defined as:
1. Absence of proteinuria (>500mg/day)
2. Absence of microhaematuria (>50RBC/hpf)
3. Normal findings on renal US
Diagnosis of exclusion- rule out prerenal/renal//postrenal causes
Incidence in cirrhotic patients with normal renal function is 18 and 39% at 1
and 5 years respectively
Neither etiology of cirrhosis nor the Child Pugh score predicts HRS
Caused by marked renal vasoconstriction causing low GFR in the face of vasodilatation of splanchnic vessels

Answer 80

A

Type 1 HRS
- Associated with doubling of serum creatinine > 2.5mg/dl (220
umol/l) or a 50% reduction in GFR to < 20ml/min in < 2 weeks. Median
survival without treatment is 2 weeks.
- Often multiorgan failure and hyponatremia
- Precipitating events: bacterial infections(specially SBP), gastrointestinal
bleeding, vigorous diuretic therapy, abdominal paracentesis or NSAIDs
Type 2 HRS
- Associated with a much less rapid decline in renal function and
mainly presents with refractory ascites.
- Median survival without treatment is
4-6 months

Answer 81

A

Terlipressin with albumin
- Vasopressin analogue Terlipressin (IV 1 to 2 mg/ 4 to 6 hourly) and albumin
given for 2 days as IV bolus (1 g/kg per day) followed by 25 to 50 grams daily up
till 15 days

Midodrine, octreotide, and albumin where terlipressin is not available
Midodrine (alpha-1 adrenergic agonist) orally at 7.5 mg tds and octreotide
(somatostatin analogue) at 100 mcg SC tds, increased as needed to 12.5 mg tds
and 200 mcg tds respectively
Norepinephrine with albumin for ICU patient with hypotension
Usually for ICU patient with hypotension
Definitive HRS treatment is liver transplantation

Answer 82

A

pregnancy
muscle mass (e.g. amputees, body-builders)
eating red meat 12 hours prior to the sample being taken

Serum creatinine may not provide an accurate estimate of renal function due to differences in muscle. For this reason, formulas were developed to help estimate the glomerular filtration rate (estimated GFR or eGFR). The most commonly used formula is the Modification of Diet in Renal Disease (MDRD) equation, which uses the following variables:
• serum creatinine
• age
• gender
• ethnicity

Answer 83

A

Derived from beta2-microglobulin (beta2-m) which is normally cleared by kidney
Beta2-m cleared poorly with low flux dialysis and PD
Somewhat better but not adequate clearance with high flux dialysis as well
Deposits particularly in bone, articular cartilage, synovium, muscle,
tendons, and ligaments
Usual presentation with BL shoulder pain/carpal tunnel syndrome
X-ray reveals bone cysts in involved bones
Switch to highly biocompatible, high-flux membrane and do longer hours
dialysis
Renal transplantation is the only definitive treatment

Answer 84

A

Proximal tubular reabsorption regulates serum P: 90% of P is reabsorbed in the proximal tubule at normal GFR
With nephron loss, remaining nephrons must excrete more P per nephron to maintain P balance
e.g., at low GFR levels, if only 10% of P is
reabsorbed, serum P can remain normal

This adaptation is mediated by phosphaturic hormones:

FGF-23 / Klotho
PTH
Reduction in 1,25-vitamin D to reduce active GI absorption

Answer 85

A

Reduced 1,25-vitamin D
Increased P
Reduced Klotho and FGF23 activity

Answer 86

A

High Phosphate
Maladaptive high FGF23
High PTH
Low 1,24 vitamin D
Low klotho

KLOTHO
- Klotho is a putative ageing suppressor gene encoding a single-pass transmembrane co-receptor that makes the fibroblast growth factor (FGF) receptor specific
for FGF-23
- Klotho is expressed in kidney distal convoluted tubules and parathyroid cells, mediating the role of FGF-23 in bone– kidney–parathyroid control of phosphate and calcium.
- Klotho−/− mice display premature ageing and chronic kidney disease-associated mineral and bone disorder
(CKD-MBD)-like phenotypes mediated by hyperphosphataemia and remediated
by phosphate-lowering interventions (diets low in phosphate or vitamin D; knockouts of 1α-hydroxylase, vitamin D receptor or NaPi-cotransporter).
- CKD can be seen as a state of hyperphosphataemia-induced accelerated ageing associated with klotho deficiency.
- Humans with CKD experience decreased klotho expression as early as stage 1 CKD; klotho continues to decline as CKD progresses, causing FGF-23 resistance and provoking large FGF-23 and parathyroid hormone increases, and hypovitaminosis.

Answer 87

A

FGF 23 requires Klotho for binding to its receptor
FGF 23 is a phosphaturic hormone that causes ventricular hypertrophy
FGF 23 is a product of osteocytes and osteoblasts

Answer 88

A

Patients with ESKD have have early loss of cortical integrity and strength that contributes to fracture risk
Cortical parameters derived from DXA images may be a useful diagnostic tool to aid in fracture prediction in patients with ESKD

Answer 89

A

a. FGF 23 decreases in chronic kidney disease stages 2 and 3

FGF23 INCREASES, KLOTHO DECREASES

Answer 90

A

d. All of the above

Answer 91

A

d. Vascular calcification is positively associated with age, time on dialysis and mortality

Answer 92

A

b. Calcium-based phosphate binders rarely cause hypercalcaemia as gastrointestinal absorption is minimal

Answer 93

A

Parathyroid hormone maintains the concentration of ionised calcium. It is synthesised and released into the circulation in response to hypocalcaemia and hyperphosphataemia. Its synthesis is inhibited by vitamin D analogues and hypercalcaemia. Parathyroid hormone has multiple systemic effects including increased bone turnover by stimulation of both osteoblasts and osteoclasts. In the kidney it decreases excretion of calcium, increases excretion of phosphate and induces 1-a-hydroxylation of calcidiol. In normal physiology, an increase in parathyroid hormone has the net effect of increasing the concentration of calcium and decreasing the concentration of phosphate.

Answer 94

A

d. Sestamibi parathyroid scanning may show a parathyroid adenoma and is advisable before surgery

Answer 95

A

a. Treatment with glucocorticoids increases the risk of hip fracture by mechanisms that include inducing osteoblast and osteocyte apoptosis

Answer 96

A

a. He should be treated with calcitriol to suppress parathyroid hormone production

Answer 97

A

d. An elevated P1NP and beta-CTx would confirm high bone turnover

Answer 98

A

Glomerular: GFR affected, albuminuria

Tubular: electrolyte and acid base disorders, water balance

Answer 99

A

E. Due to their action in the distal nephron, thiazides are more likely than loop diuretic to cause dilutional hyponatremia

Answer 100

A

Methotrexate
Acyclovir
Vit C
Insoluble drug in urine - form crystals

Answer 101

A

Drug-uromodulin interaction - cast formation

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