Kidney disease

Question 1

How is filtrate formed in the kidneys?

Answer 1

The renal corpuscle forms the filtrate from blood that is free of cells, larger polypeptides and proteins
This filtrate then leaves the renal corpuscle and enters the tubule
As it flows through the tubule substances are added or removed from it e.g. salts (NaCl), urea
Ultimately, the fluid remaining at the end of each nephron combines in the collecting ducts and exits as urine.

Question 2

What are the four processes that occur in the kidneys?

Answer 2

• Filtration
• Reabsorption
• Secretion
• Excretion

Question 3

What is the structure of the nephron

Answer 3

Bowman’s capsule
Loop of Henle –> consists of a descending limb from the proximal tubule and an ascending limb leading to the distal convoluted tubule
- Counter current multiplier system –> two different directions, left hand side very permeable to water, encourages water reabsorption facilitated by aquaporins. Right hand side, not very water permeable, NaCl reabsorption.
Fluid flows from the distal convoluted tubule into the collecting ducts system, which is composed of the cortical collecting-duct system

Question 4

What does the kidney control?

Answer 4

Total body water
Electrolytes - Na, Ca and Mg –> reabsorbed
- K –> absorbed
pH –> 7.4
Nitrogenous waste materials –> urea

Endocrine
- Erhyropoietin –> link to blood volume, kidney stimulate RBC production from stem cells if volume low
- Renin –> blood pressure regulation
- Vitamin D –> calcium absorption from gut

Question 5

How do the kidneys help with blood pressure control?

Answer 5

Blood pressure regulation is determined by cardiac output and diameter of blood vessels/ resistance.
Blood vessel diameter and resistance involves renin which is released by the kidneys
The more your heart pumps out and the smaller the bv diameter the higher the blood pressure
Control of fluid volume in the blood will have an affect on bp. The more fluid the higher the bp

Question 6

Discuss the renin-angiotensin-aldosterone system
Mechanism

Answer 6

Juxtaglomerular apparatus responds to 3 types of stimulation
- reduced salt
- reduced pressure
- adrenoreceptor stimulation
In response to this the kidney releases renin –> an enzyme which enters the blood stream

At the same the liver is producing Angiotensinogen

Renin cleaves Anigotensinogen to form Angiotensin 1 which remains in circulation around the lungs.
The lungs produce an enzyme called ACE which then helps with mediating bp
ACE cleaves Angiotensin 1 to Angiotensin 2

Angiotensin 2 can bind to a number of different cell receptors and stimulate a number of processes
- Sympathetic activity
- Increase the number of proteins to be embedded into the tubular causing an increase in Na reabsorption, passive affect is then absorbing more H2O (can also be hormone stimulated - aldosterone) Also stimulates K excretion and Cl reabsorption
- Adrenal gland secretes aldosterone, lipid based steroid hormone (can diffuse across plasma membrane quickly)
- Arteriolar vasoconstriction –> increase in blood pressure
- ADH mediated secretion mediated by the pituitary gland causing H2O absorption in the collecting duct

Mechanisms are in place to reduce the physiological strain on the body which caused the body to produce renin in the first place.
Occurs in normal physiological states

Question 7

What is the rate of glomerular filtration?

Answer 7

The volume of fluid filtered from the glomeruli into Bowman’s space per unit time is known as glomerular filtration rate (GFR)
GFR is determined by net filtration pressure, the permeability of the corpuscular membranes, osmotic force of any proteins there, and the surface area available for filtration. Large surface area helps with effectiveness

Average person –> renal blood flow is 180L/day / 125ml/ min

Total plasma volume in the circulatory system is around 3L, so the kidneys filter the entire plasma around 60 times per day. Efficient mechanism for waste product removal as it filters so quickly
This allows the kidneys to rapidly regulate the constituents of the internal environment and excrete large quantities of waste products

Question 8

What is acute kidney injury?

Answer 8

AKI is defined as an abrupt (within hours) decreases in kidney function, which encompasses both injury (structural damage) and impairment (loss of function)
- AKI is the same as acute renal failure

It is a syndrome that rarely has a sole and distinct pathophysiology

Many patients with AKI have a mixed aetiology where the presence of sepsis, ischaemia and nephrotoxicity often co-exist and complicate recognition and treatment

Question 9

What are the causes of AKI?

Answer 9

Pre-renal –> relate to decreased perfusion pressure

Post-renal –> obstructive

Intrinsic –> related to pathology of the vessels, glomeruli, or tubules-intestitium

If the Pre and or post renal conditions persist, they will eventually evolve to renal cellular damage and hence intrinsic renal damage

Question 10

What are the intrinsic causes of AKI?

Answer 10

Tubular
- Renal ischaemia –> e.g. complication of surgery, pancreatitis, pregnancy, trauma
- Nephrotoxic drugs –> antibiotics, antineoplastic drugs, anaesthetic drugs, heavy metals
- Endogenous toxins –> myoglobin, haemoglobin, uric acid (in proper breakdown can be toxic)

Glomerular
- Acute post-infectious glomerulonephritis
- Lupus nephritis
- IgA glomerulonephritis

Interstitium
- Infections –> bacterial, viral
- Medications

Vascular
- Large vessels –> bilateral renal vein thrombosis
- Small vessels –> vasculitis, malignant hypertension, atherosclerosis

Question 11

How can AKI lead to multi-organ injury?

Answer 11

AKI leads to distant organ injury through a combination of pro-inflammatory and oxidative stress-mediated mechanisms

Serum and distal organ cytokine levels (IL1, IL6, IL10 and TNFa) cause an increase in immune system response by increase leukocyte trafficking (neutrophil, lymphocyte and macrophage) and increased oxidative stress (glutathione depletion).

In addition, sodium and water channel dysregulation in the lungs in aggravate pulmonary oedema.

Question 12

What is chronic kidney disease?

Answer 12

Presence of kidney damage or estimated glomerular filtration (eGFR) less than 60ml/min/1.73m2, persisting for 3 months of more, irrespective of the cause. –> 50% of functional reserve from kidney lost (normal value 120)

Progressive loss of kidney function ultimately resulting in the need for renal replacement therapy (dialysis or transplantation)

Kidney damage refers to pathologic abnormalities either suggested by imaging studies or renal biopsy abnormalities in urinary sediment or increased urinary albumin excretion rates.
Patients rarely recover from CKD

Chronic and sustained insults from chronic progressive nephropathies (cause loss of function) evolve to progressive kidney fibrosis and destruction of the normal architecture of the kidney.
This affects all 3 compartments, mainly glomeruli, the tubules, interstitium and the vessels.
It manifests histologically as glomerulosclerosis (scaring), tubulointerstitial fibrosis and vascular sclerosis

Question 13

What are the units of GFR?

Answer 13

ml/min/1.73m2

Question 14

What is the pathophysiology of of CKD?

Answer 14

Chronic and sustained insults from chronic progressive nephropathies (cause loss of function) evolve to progressive kidney fibrosis and destruction of the normal architecture of the kidney.
This affects all 3 compartments, mainly glomeruli, the tubules, interstitium and the vessels.
It manifests histologically as glomerulosclerosis (scaring), tubulointerstitial fibrosis and vascular sclerosis.
Reduced glomerular surface area which affects glomerular filtration rate.

The sequence of events which lead to scarring and fibrosis are complex, overlapping and are multistage phenomena.
Infiltration of damaged kidneys with extrinsic inflammatory cells
Activation, proliferation and loss of intrinsic renal cells through apoptosis, necrosis etc
Activation and proliferation of extracellular matrix e.g. connective tissue, producing cells including myofibroblasts (usually disappear during wound healing) - don’t undergo normal apoptosis
- Deposition of ECM replacing the normal architecture

Inflammatory cascade

Question 15

What are the 5 stages of CKD and linked GFR?

Answer 15

Stage 1
- eGFR –> 90 or more ml/min/1.73m2
- Normal kidney function but with some kidney damage or disease
- e.g. Protein or blood in urine, kidney inflammation

Stage 2
- eGFR –> 60-89ml/min/1.73m2
- Mildly reduced kidney function AND you are already to have some kidney damage or disease.
- People with a eGFR or 60-80 without any known kidney damage or disease are not considered to have CKD

Stage 3 A & B
- eGFR –> A = 45-59ml/min/1.73m2 B = 30-44ml/min/1.73m2
- Moderately reduced kidney function –> with or without known kidney disease

Stage 4
- eGFR –> 15-29ml/min/1.73m2
- Severely reduced kidney function

Stage 5
- eGFR –> <15ml/min/1.73m2
- Very severely reduced kidney function
- Sometimes called end-stage kidney failure or established renal failure

There is an increased plasma concentration of Cystatin C with kidney damage as it is usually removed when kidney working healthily
High levels of creatinine also indicate CKD as its usually filtered out.

Question 16

How does GFR change with age and disease?

Answer 16

Rate of kidney disease progression increases with age and disease.
Early detection helps with patient outcome. Depends on whether it is treated or untreated.

In diabetic patients
If CKD is treated when GFR reaches 60, patient is given an extra 10 years.
- untreated would give the patient 5 years

Question 17

GFR vs Creatinine
What is their relationship?

Answer 17

Serum creatinine levels rise with decreasing GFR
However care is needed when interpreting results since the relationship between serum creatinine concentration and GFR is logarithmic rather than linear.
- meaning in terms of GFR, small creatinine changes at low levels indicate a similar decline in GFR to large changes in creatinine at high levels.
Since creatine is produced as a by-product from muscle turnover, care to interpret results in individuals with low muscle bulk e.g. elderly or underweight
- because of low rate of creatinine productions, their GFR will be significantly lower than suggested by their serum creatinine level

Large change in GFR but little change in creatine (early renal disease).
Large change in plasma creatinine but little change in GFR (advanced renal failure)

Question 18

How is albuminuria used for diagnosis?

Answer 18

Albuminuria is concentration of albumin in kidney.
In a damaged kidney albumin passes from the bloodstream into the urine where in a healthy individual it is not present.
A blood sample for creatine and urine sample for albumin can be crucial in kidney disease diagnosis.

There are three levels of albuminuria which include an albumin-creatinine ratio (ACR) –> when putting GFR with ACR (mg/mmol) adverse outcome risk can be predicted when reading both values of a combined risk chart.
e.g. a ACR of 40 is ‘severely increased’ but with a GFR between 60-89 it is overall moderate - severe

Question 19

What are some of the causes of CKD?

Answer 19

• Type 2 diabetes (30-50%)
• Type 1 diabetes (3.9%)
• Hypertension (27.2%)
• Primary glomerulonephritis (8.2%)
• Chronic tubuloinerstitial nephritis (3.6%)

CKD may results from disease processes of there categories, same as in AKI
- Pre-renal –> decreased renal perfusion pressure
- Intrinsic renal –> pathology of vessels, glomeruli, or tubules-interstitium
- Post-renal –> obstructive

Question 20

What are some non-modifiable risk factors for CKD?

Answer 20

• Older age
• Males
• Ethnicities such as African Americans, Afro-Caribbean, Hispanics and Asians
  Genetic factors –> increase susceptibility
• Single nucleotide polymorphisms in the genes TCF7L2 and MTHFS were associated with diabetic nephropathy and CKD progression
• Polymorphisms of genes coding for mediators of renal scarring and renin-angiotensin-aldosterone were found to influence CKD progression
  Unsurprisingly the systems that control homeostasis of the kidney, if affected, will increase the likelihood of CKD.

Question 21

What are some modifiable risk factors for CKD?

Answer 21

• Systemic hypertension
• Proteinuria
• Diabetes

Question 22

What symptoms are linked to each stage of CKD?

Answer 22

Stage 1
- Some protein in urine
- Largely there can be no symptoms
- 90-60% remaining kidney function

Stage 2
- Proteinuria
- Physical damage to kidney
- 60-40% remaining kidney function

Stage 3 A and B
- Swelling in hands and feet
- Back pain
- Frequent urination
- Anaemia
- High blood pressure
- Bone disease
- Can be slowed by controlling blood sugar levels of they have diabetes, controlling BP, not smoking, being active, maintaining moderate weight.
- Dietitian referral
- 40-20% remaining kidney function

Stage 4
- Same symptoms as 3 but more severe
- May be referred to a nephrologist and dietitian
- ACE inhibitor prescription
- 20-10% remaining renal function

Stage 5
- Close to failure
- Itching
- Muscle cramps
- Nausea
- Vomiting
- Swelling
- Back pain
- Frequent urination
- Difficulty sleeping and breathing
- Undergo dialysis and transplant
- 10-0% remaining kidney function

Question 23

What is the prevalence of CKD?

Answer 23

In UK it is estimated >3.5 million people age 18 and over have stage 3-5 CKD
Worldwide prevalence is estimated to 8-16% –> number probably higher due to many not being diagnosed
Prevalence will be higher in those with other conditions linked to CKD such as diabetes and hypertension.

Question 24

How can CKD be prevented?

Answer 24

Glycaemic and blood pressure control
- especially in those with diabetes and hypertension
Control of cholesterol
- especially in those with high LDL levels
Correction of acidosis?
- if low a vegetarian diet/ high consumption of fibre/ low consumption of animal proteins can help to try and raise it

Question 25

What is the treatment of CKD?

Answer 25

Very few cases are amenable to curative treatment, therefore the aim is to slow the rate of decline in renal function and limit associated complications.

Dietetic treatment
- Restriction of dietary intake can minimise biochemical effects of reduced renal function
- However, nutritional support will also be a priority since malnutrition is prevalent in the patient group

Important in stages 1-3 to promote a healthy diet to control the consumption of animal protein, promote physical activity, weight control and reduce smoking.
Medication usually introduced in stage 4

Question 26

What is haemodialysis?

Answer 26

When blood is pumped out of the body to an artificial kidney machine and returned to the body by tubes that connect the patient to the machine.
Dialysis machine acts an artificial kidney where various components are filtered out of the blood through a semi-permeable membrane
Often for those waiting for a kidney transplant
- waiting list on average is 2 and a half to 3 years

Question 27

What is peritoneal dialysis?

Answer 27

2 types

Continuous Ambulatory Peritoneal Dialysis
- Continuous, machine free process which can be done whilst undertaking normal daily activities
- 2 litres of cleansing fluid goes through a tube into the belly where an exchange occurs and then the fluid is drained out of the belly and thrown away.

Automated Peritoneal Dialysis
- Machine delivers and drains cleansing fluid
- Usually done whilst asleep

Question 28

What are the pros and cons of Haemodialysis?

Answer 28

Pros
- Predictable ultrafiltration with each session
- Frequent evaluation of volume status by health-care provider
- Variety of therapeutic interventions to manage intradialytic hypertension

Cons
- Haemodynamic instability, particularly in presence of ventricular dysfunction
- Myocardial stunning with aggressive ultrafiltration

Question 29

What are the pros and cons of peritoneal dialysis?

Answer 29

Pros
- Gentle and sustained fluid removal
- Better preservation of residual renal function
- Ability to use cardioprotective medications with lower risk for hyperkaelemia

Cons
- Precise predictions of daily ultrafiltration volume not possible
- Greater dependence on patient to adjust prescription in response to daily fluid status fluctuationa

Question 30

What are the different types of kidney stones?

Answer 30

Calcium stones
- formed due to an excess of oxalate –> found in some fruit, veg, nuts and chocolate
- oxalate has a -2 charge so binds readily to Ca2+
- 75%

Struvite stones
- less comon
- caused by an UTI
- can grow quickly and become quite large
- 10-15%

Uric acid stones
- due to chronic dehydration
- risk increases with those with gout, a genetic tendency or a diet too high in protein
- 5-10%

Cystine stones
- formed in those with an inherited disorder than causes the kidneys to excrete an excess of certain amino acids
- 1%

Xanthine stones
- caused by an enzyme deficiency that causes the build-up of xanthine deposists

Silica stones
- rare
- caused by certain medications or herbal supplements

Calcium and struvite have a composition mainly from element that can precipitate
Others have a genetic component
Kidney stones can be asymptomatic

Question 31

What are the prevalence of kidney stones?

Answer 31

Present at some time 1 in 10
Men more affected than women
Peak age is between 30-50

Question 32

What are the risk factors for getting kidney stones?

Answer 32

• Anatomical anomalies in kidneys and/or urinary tract
• Family history
• Metabolic disorders which increase excretion of solutes e.g. chronic metabolic acidosis, hypercalciuria
• Deficiency of citrate in urine –> often prescribed to break them down
• Medications e.g. diuretics, calcium/ vitamin D supplementation

Lifestyle
- Hypertension
- Gout
- Immobilisation
- Relative dehydration
- Elevated animal product consumption

Question 33

What are the symptoms of kidney stones?

Answer 33

Most asymptomatic
Can have severe pain –> starts in loin and moves to groin
Sometimes haematuria

Question 34

How are kidney stones diagnosed?

Answer 34

Stick urine testing
- RBC, WBC, nitrates, pH
- Collect urine over 24hour for analysis
- Non-specific test, usually coupled to symptoms

Non-enhanced CT scanning
- The imaging modality of choice has replaced Intravenous Pyelogram
- Non-invasive
- Detects 90-95% of KS

Plain X-rays of kidney, ureter and bladder
- Useful to watch the passage of radio-opaque stones (75% of stones are calcium so will be radio-opaque)

Question 35

Who is recommended for kidney stone analysis?

Answer 35

• All first-time stone formers
• All patients with recurrent stones who are on pharmacological preventing treatment
• Patients who have had early recurrence after complete stone clearance
• Late recurrence after a long stone free period

Patients encourages to try and catch the stone by filtering urine through a tea strainer or filter paper.

Question 36

What is the treatment for kidney stones?

Answer 36

Non-invasive
- NSAIDs –> Diclofenac
- Provide antiemetics and rehydration therapy –> can help stone to pass the urinary tract
Majority of stones will pass spontaneously within 1-3 weeks

Invasive
- Extracorporeal shock wave lithotripsy –> sound waves
- Percutaneous nephrolithotomy –> a needle breaking it down
- Uteroscopy
- Open surgery

Question 37

How does nutrition affect kidney stone formation?
Any dietary advice?

Answer 37

High meat consumption linked to formation

Advice
- Low oxalate diet
- Getting enough dietary calcium
- Reduce salt intake
- Limit animal protein
- Drink more fluid