Cases Semester II Flashcards
- A 25-year-old woman has been admitted because of a severe dyspnea of sudden onset. She mentions that she wakes up at night because of coughing lately. She also noticed a wheezing sound occasionally, during respiration. She is allergic, she has been smoking for 5 years, 5 cigarettes/day.
Physical examination: diaphragm is found low by percussion, exhalation is prolonged, with a bit of wheezing at the end.
Pulmonary function tests:
- *FVC:** 3.02 l (80%)
- *FEV1**: 1.52 l (45%).
Reversibility test with Salbutamol:
- *FVC**: 3.52 (95%)
- *FEV1**: 1.75 l (62 %)
What is the most likely diagnosis?
- Pulmonary function test is low
- Reversibility test: there is improvements of FEV1 after salbutamol (bronchial dilator):
the obstruction is temporarily and reversible. Suggest asthma.
- Key: allergy frequently precedes development of asthma.
- FVC > 80 %
- FEV1: > 80 %
- Symptoms of asthma: chronic inflammatory disorder of the airways
o Recurring episodes of wheezing, breathlessness, chest tightness, and coughing, particularity at night or in the early morning.
Paroxysmal nocturnal dyspnea is due to respiratory depression during sleep worsening the already present pulmonary issues
the minimum difference in % between FVC taken before and after Reversibility test to make a confident diagnosis of asthma. The answer is 15%.
TYPES
atopic,
non-atopic,
drug-induced
and occupational asthma.
o Risk factors: house dust mites, animals with fur, pollens, respiratory (viral) infections, exercise, strong emotional expressions, chemical irritants, drugs (such as aspirin and beta blockers) etc.
A 67-year-old man complains of coughing. He is currently producing a lot of yellowish- greenish sputum, that is more than the amount he usually has. It is hard for him even to get to the toilet, because of his severe dyspnea. He has been treated for hypertension and hyperlipidemia for years. He weighs 100 kg. He has been smoking since the age of 14, around 30 cigarettes/day.
Physical examination: his lips are markedly cyanotic, exhalation is prolonged with occasional wheezing at the end. Bronchial ronchi can be heard.
ABG:
pH: 7.35
pCO2: 43 mmHg
pO2: 54 mmHg
Pulmonary function tests:
FVC 2.12 l (52 %)
FEV1: 0.97 l ( 32%)
TLC: 5.24 l (105%)
RV: 3.27 (176%) Raw: 0.87 kPa·s/l.
Reversibility test with Salbutamol:
FVC: 2.19 l (54%)
FEV1: 1.01 l (33 %)
What sort of ventilatory defect is present? What is the most likely diagnosis?
Calculated TI = 62%
Semi-old man, buckets of sputum, 80 pack years.
High risk of COPD, symptoms of Chronic Bronchitis
Cyanosis, prolonged exhalation and wheezing fit with obstructive disease
Should check chest diameter, patients with Chronic Bronchitis can have a “barrel chest” (barrel chest + cyanosis → “Blue Bloater” chronic bronchitis phenotype)
- In this case he has increased amount of sputum: looks like an acute upper respiratory inflammation
- Suggest obstructive lung disease: blue bloater?
- pO2: low
- pCO2: not so high, should be high in chronic bronchitis.
- There is an acute worsening of the condition: probably hyperventilation, that brings pCO2 back to near normal.
- Pulmonary function test: very bad
o FVC and FEV1: is very low
o TLC and RV: is increased
o RAW: resistance of airways: probably low.
- Reversibility test: no difference, which means it is not asthma.
- Ventillatory defect: obstructive disease
- Chronic bronchitis, with acute worsening of the condition.
- Chronic bronchitis
Raw = Rairway isn’t really mentioned elsewhere, but Hamar says we only need to know that it is an abbreviation for airway resistance, and it’s increased because of the obstruction.
Salbutamol-test shows 2% and 1% increase in FVC and FEV1, disproving asthma
Diagnosis: Severe COPD
o Chronic cough associated with sputum production more than 90 days on 2 successive years.
o Cause:
Smoking, air pollution, occupational exposure, etc.
- A 55-year-old woman complains of hardening of her skin, having fissures on her hands. She has been avoiding climbing stairs for years due to breathlessness. Her dyspnea got much worse in the last few years. Auscultation of the lungs does not reveal any abnormality. Chest radiography shows increased opacification on both sides, mostly at the bases, above the diaphragm. The heart appears enlarged to the right, the pulmonary trunks are thicker on both sides.
Pulmonary function tests:
FVC: 3.01 l (64 %)
FEV1:2.75 l (68%)
TLCO:54 %
KLCO: 45%
ABG at rest (Arterial Blood Gas) :
pH: 7.38
pCO2: 38 mmHg
pO2: 81 mmHg
ABG after 6 min of exercise:
pH: 7.42
pCO2: 34 mmHg
pO2: 75 mmHg
ECG: signs of right ventricular strain, P pulmonale
What sort of ventilatory defect is present? What additional tests should be performed? What is the possible diagnosis?
Middle-aged woman, hardening skin and fissures could be CREST/Scleroderma[1]
Progressively worse exertional dyspnoea could be anything, but fits with Scleroderma
CXR shows bilateral opacification of the bases of the lungs which is indicative of interstitial lung disease
The RVH is due to pulmonary hypertension caused by the chronic pulmonary fibrosis
Pulmonary Function tests show decreased FVC, FEV1 and increased TI
FEV1 ≤ 80%, FVC ≤ 80% and TI ≥ 70% is indicative of restrictive disease
This fits with scleroderma
TLCO (Transfer factor of the Lung for CO) is aka DLCO
(Diffusion lung capacity for CO). (normal is 81-140%)
This is the result of a Gas Transfer Test, using CO because it has a similar diffusion capacity to O2.
TLCO is decreased in any condition which affects the effective alveolar surface area, this patient’s decreased TLCO fits with Scleroderma
KLCO (TLCO corrected for alveolar volume) should be lower than TLCO.
A KLCO that is higher than TLCO indicates that the restriction is extrapulmonary.
In this this patient the KLCO is lower than TLCO disproves extrapulmonary restriction (obesity, kyphoscoliosis, ascites)
ABG:
paO2 is decreased in rest. Exercise shows that compensation to strain is insufficient.
paCO2 decreasing below normal values (35-45 mmHg) shows that she is hyperventilating. CO2 has a much higher diffusion capacity than O2, because of the pressure-gradient, and so is easily “excreted” even though she has a reduced alveolar volume. However O2 hit its diffusion capacity even before exercise (she was hypoxemic at rest), and paO2 continues to decrease.
ECG: RV strain due to hypoxia, p pulmonale due to pulmonary HTN, which again, is caused by the pulmonary fibrosis
Dx:Pulmonary tests, ABG and ECG point to Interstitial Lung Disease, which could be explained by systemic scleroderma (Autoimmune hyperproduction of Collagen[2] ).
Check autoantibodies to confirm (local form has anticentromeric Ab, diffuse has anti-topoisomerase Ab) also anti-RNAP 3
Systemic Scleroderma reaching the lungs indicates a 70% 5-year survival
There is no cure, however it was mentioned that you can treat/ alleviate symptoms with anti-fibrotic drugs and immunosuppressants.
CREST refers to limited scleroderma, just from the fact that there is hardening of skin cant exclude it. But because of the lung involvement this is systemic (diffuse) scleroderma.
autoimmune disease leading to fibroblast overactivation -> overproduction of collagen
- Some weeks after having a sore throat and high fever, the patient has developed edema. His blood pressure is increased.
Urinalysis:
- *volume:** 450 ml/day !!!
- *protein**: +++ (3 g/day)
- *sediment**: 50–100 erythrocytes/HPF, leukocytes rarely
- *creatinine clearance**: 30 ml/min
What is the presumable diagnosis?
Low urine volume (normal: 1-1.5L/day)
Considered oliguria because it’s between 200 and 500 mL/day. Below 200 mL is considered anuria.
+++ = Large proteinuria
(normal is 50-150 mg/day. Pathological if > 300mg/day. Considered “massive proteinuria” if > 3 g/day)
Causes edema from the reduced capillary colloid osmotic pressure
Sediment shows hematuria / significant red blood cells in the urine
(considered microscopic hematuria is >3 RBCs per high power field)
Very Low GFR (normal creatinine clearance is 120-125 mL/min)
Kidneys are failing to properly filter the blood, probably due to glomerular inflammation
Low GFR ⇨ water retention ⇨ hypertension, both of which also contribute to edema
Diagnosis: Nephritic Syndrome based on hematuria
(if it was only protein and no blood, then it would be nephrotic syndrome)
Probably due to post-streptococcal glomerulonephritis
(upper respiratory infection, then weeks later ⇨ glomerulonephritis with immune complex deposition in glomeruli, between the basement membrane and podocytes. Immune complexes activate the complement system, causing inflammation and damage to the filtration barrier, allowing proteins to leak into the urine)
- Laboratory findings of a patient with massive edemas:
serum total protein: 40 g/l
serum cholesterol: 10 mmol/l
ESR: 28 mm/h
blood pressure: 125/80 mmHg
Urinalysis:
quantity: 1800 ml/day
protein: ++++ (12 g/day)
sediment: 1–2 leukocytes/HPF, erythrocytes rarely, a lot of hyaline casts
What is the presumable diagnosis?
Very Low Serum Protein (normal is 60-80 g/L)
Causes edema due to reduced capillary colloid osmotic pressure
High Serum Cholesterol (normal 3.6-5.2 mmol/L)
Exact mechanism of why this occurs is unclear, but whenever the kidney loses a lot of proteins, the liver synthesizes more proteins - including VLDL. Also LDL is probably big enough to not be filtered by the kidney, and so remains in the bloodstream.
Increased ESR (normal is < 20 mm/hour)
Low serum protein means there are fewer negative charges in the blood (especially due to albumin loss), and those charges normally repel the negative charges on the RBCs. This repelling effect (or “zeta potential”) normally makes the rate at which RBCs settle (erythrocyte sedimentation rate) fairly slow. With reduced zeta potential, red blood cells are able to settle at a faster rate (Zeta Potential↓ = ESR ↑)
Normal Blood Pressure (helps rule out other causes of edema besides proteinuria)
Normal Urine Volume (normal is 1-1.5 L/day) Technically this is higher than the 1.5 L/day range on their lab values sheet, but only 300 mL more is not significant.
Massive Proteinuria (normal is < 300 mg/day, and it’s already considered massive proteinuria at > 3 g/day… 12 is very high)
No hematuria: Only a few RBCs seen
Diagnosis: Nephrotic syndrome based on massive proteinuria with edema, hyperlipidemia, and no blood in the urine. Doesn’t tell you anything about what could have caused the nephrotic syndrome.
Extra: Possible causes of nephrotic syndrome:
Primary Glomerulonephrosis:
effects limited to kidney; many different causes + histological manifestations; mostly due to immune complex deposition (often autoimmune), toxins or drugs.
Secondary Glomerulonephrosis: systemic effects with kidney involvement
Diabetic Nephropathy - renal damage from hyperglycemia, AGE
Auto-immunity - seen in SLE (“lupus nephritis”), Sjogren’s, AI vasculitis; immune complex deposition → renal damage
Infections - syphilis, Hep B, HIV
Multiple Myeloma - accumulation/precipitation of light chains → cast formation → obstruction + toxicity
Other Cancers - invasion of glomeruli by cancer cells
Amyloidosis / Sarcoidosis - accum. of amyloid / inflamm. granulomas, respectively (renal involvement rare, but possible, in sarcoidosis)
Genetic - congenital nephrotic syndrome, mutated nephrin filtration barrier protein
Drugs - penicillin, captopril
- A febrile patient complains of lumbar pain.
Urinalysis:
protein: ++
pus: +++
sediment: a lot of leukocytes, some erythrocytes, epithelial cells, a lot of bacteria, leukocyte casts
CK: 100 ml/min
ESR: 38 mm/h
What is the presumable diagnosis?
Moderate protein in urine: (normal < 300 mg/day / day). Some glomerular damage
Pyuria: pus in urine, sign of urinary tract infection (E.coli , enterofaecalis)
Leukocytes in urine indicates infection, while RBCs and epithelial cells indicate damage
Leukocyte casts indicate pyelonephritis, as they are made in the tubular system.
Slightly Low CK: some impaired kidney function
Increased ESR: (normal is < 20 mm/hour)
ESR normally is increased with inflammation due to acute phase protein synthesis, specifically that the increased serum fibrinogen causes RBCs to clump together and settle at a faster rate.
Diagnosis: Pyelonephritis.
Pyelonephritis usually is the result of **ascending urinary tract infection.
Lumbar pain**
occurs due to inflammation distending the renal capsule, and fever occurs due to organ infection stimulating systemic cytokine responses.
Examples include
albumin,[5]
transferrin,[5]
transthyretin,[5]
retinol binding protein,
antithrombin,
transcortin.
The decrease of such proteins may be used as markers of inflammation. The physiological role of decreased synthesis of such proteins is generally to save amino acids for producing “positive” acute phase proteins more efficiently.
Theoretically, a decrease in transferrin could additionally be decreased by an upregulation of transferrin receptors, but the latter does not appear to change with inflammation.
- Laboratory findings of a patient include the following:
Urinalysis:
sediment: 3–5 erythrocytes/HPF, rarely leukocytes;
the erythrocytes are isomorphic;
minimal proteinuria; -the urinary protein electrophoresis does not show selectivity in the proteinuria
Ck: 120 ml/min
What can be the probable diagnosis: glomerular hematuria or urinary tract bleeding?
Diagnosis: Mild Urinary Tract Bleeding, probably from kidney stone (nephrolithiasis)
Slight Microscopic Hematuria: normal is < 3 erythrocytes / HPF
Normal Morphology (Isomorphic) RBCs: indicates the bleeding occurs more distally in the urinary tract
If there is glomerular damage where red blood cells enter the tubules for filtration, then the cells are present during the concentrating process, which dehydrates them ⇨ small, dysmorphic erythrocytes. That did not occur here, so the glomeruli and tubules are probably fine.
Minimal proteinuria: the equipment is not sensitive enough to show proteinuria < 300 mg / day : also suggest that it is not a glomerular bleeding, always goes together with a significant proteinuria
“No selectivity in the proteinuria”: since bleeding is likely distal in the urinary tract, no filtration barrier is involved. Blood leaks into the urine, and so all proteins can get in.
Normal Creatinine Clearance: GFR is not impaired
- After receiving a massive dose of aminoglycoside antibiotic, a patient with no prior symptoms of kidney disease develops a body weight gain of 3 kg over a period of 3 days. He does not void urine spontaneously. The total volume of urine collected by catheterization is 200 ml/day.
Other laboratory results:
serum creatinine: 440 μmol/l NB!!!
serum urea: 28.5 mmol/l +
plasma K : 6.2 mmol/l
What is the most likely diagnosis?
Tubular damage: Aminoglycosides are known to be toxic to the renal tubules
Weight gain due to water retention from extremely low urine output
Anuria < 200 mL urine / day
3 serum metabolite levels are all elevated, indicating retention due to renal failure:
Elevated serum creatinine: (normal 40-130 µmol/L)
Elevated serum urea: (normal 2 - 10 mmol/l)
blood urea nitrogen (BUN) is ‘carbamid’ on the pathophys ref. ranges document)
Hyperkalemia: (normal Se [K+] 3.5-5 mmol/L)
Diagnosis: Acute Renal Failure (ARF) due to aminoglycoside toxicity
- The serum glucose level is 15 mmol/l in a diabetic ketoacidosis.
GFR is markedly decreased (20 ml/min).
Tubular function tests are negative.
No glucose can be detected in the urine (by repeated tests).
How is this possible?
- If the GFR is decreased enough, the glucose load is also decreased.
Normally, glucose is reabsorbed in the tubules up until it reaches the BGL concentration of 10 mmol/L, at which point the SGLT transporters are saturated
In this case, the GFR is so low that glucose has time to be reabsorbed in the tubules by SGLT2 transporters, which are not damaged
- Less glucose per time is filtered into the renal tubules. This gives the patient _more time to reabsorb the glucos_e. Thus, glucosuria will not develop.
- If the GFR is very low, the patient will have a higher tubular threshold and the glucose will not be detected in the urine.
- Tubular function test: negative
-Concentration + dilution test: follow up!
Concentration test:
dinner without fluid and no drinking of fluid throughout the
night: urine in the morning is analyzed for its density. If the urine in morning is
not concentrated, it means that something wrong. It should be increased.
- *Dilution** test: drink 1-2 L tea or a large amount of fluid; then the urine sample should have low-density values, and low osmotic cc.→ If the urine is not diluted, so it does not go below 1,010 kg/l (density→ there is a problem with dilution of the urine
- Patient with chronic renal disease loose first the concentration capability and later they loose the dilution capability (end stage: cannot concentrate nor dilute – the urine osmolarity is the same as the urine – called isostenuria.
- Laboratory findings of a patient:
Urinalysis:
color: straw-yellow
transparency: turbid (nubecula)
quantity: 400 ml (present), 1600 ml/day
specific gravity: 1022
protein: 50mg/day
pus: +++
blood: +
glucose: neg
acetone: neg
ubg: norm
bilirubin: neg
Urinary sediment:
20–30 epithelial cells
30–40 WBC
3–4 RBC, per high power field
Further data:
body temperature: 38°C
WBC: 12 G/l
RBC: 4.5 T/l
ESR:2 mm/h
creatinine clearance: 120 ml/min,
cultivation of E. coli: positive
What is the most likely diagnosis?
Many normal findings are listed:
normal urine volume (being just above the “normal” 1.5L/day is not significant), normal specific gravity (1010-1035), no proteinuria (< 300 mg/day), no glucosuria (no diabetes), normal UBG and bilirubin (liver is OK), body temperature on the upper end of normal but it’s not a true fever, normal RBC count (4.4-5.5 T/l), ESR is < 20 mm/h, normal creatinine clearance (120-125 ml/min)
Diagnosis: Urinary Tract Infection from E. coli that has not ascended to become pyelonephritis
Color: seems to indicate significant pus
Pus +++: clear sign of infection
Microscopic hematuria: very small amount of blood. Never find out if RBCs are isomorphic for sure but they probably are since there is no renal glomerular/tubular involvement.
Epithelial cells in urine: also due to damage
Elevated WBC count: (normal 4-10 G/l) - usually increases with infection
Neutrophils in particular increase with bacterial infections
Positive E. coli Culture: makes the diagnosis of UTI easy.
No signs of systemic/organ infection → ESR is not elevated, no fever, etc.
Urinary tract infections do not normally cause fever unless the infection reaches the kidney.
- A 56-year-old woman complains of fatigue. According to her medical records, she has hypertension, peptic ulcer and nephrolithiasis.
Laboratory findings:
serum Ca: 2.8 mmol/l
serum phosphate: 0.6 mmol/l
serum ALP: 450 U/l
DEXA scan: T-score of –2.8 SD on the hip and forearm.
What test(s) would you order to determine the exact cause of her disease?
Elevated serum [Ca2+] (normal: 2.2-2.6 mmol/L)
- High serum calcium can be cause of nephrolithiasis (kidney stones) and fatigue
Low serum [Pi] (normal: 0.8-1.45 mmol/L, although it’s not listed on the lab values sheet)
Elevated serum ALP (normal: < 150 U/L)
- In this situation, high ALP probably indicates increased osteoblast activity
ALP is usually normal in people with primary osteoporosis, and so this is an indicator that here there is a problem with hyperparathyroidism ⇨ osteoclast bone resorption ↑
Osteoporotic T score (normal > -1.0, low bone mass/osteopenia if -1.0 to -2.5, osteoporosis if < -2.5)
T score is the patient’s bone density compared (by standard deviation) to the bone density of a young population (30 years old). It is measured by DEXA: Dual Energy X-ray Absorptiometry
Probable Diagnosis: Primary Hyperparathyroidism
(intrinsic oversecretion of PTH from parathyroid gland. Can be caused by adenoma or hyperplasia) Osteoporosis because of PTH ⇨ osteoclast activity ↑, bone resorption ↑
- Note that this is secondary osteoporosis, because osteoporosis is only “primary” if it’s the common postmenopausal, age-dependent kind
PTH increases osteoclast activity ⇨ Ca2+ ↑
PTH induces increased production of vitamin D + induces kidney to increase calcium reabsorption and phosphate excretion ⇨ [Ca2+] ↑↑, [Pi] ↓
Hypercalcemia frequently induces increased gastrin secretion that may cause hyperacidity and thus be the cause of the peptic ulcer
(Gastrin stimulates parietal cells to secrete more HCl)
Additional tests to determine disease:
Scintigraphy with 99mTc to check parathyroid function,
imaging for neoplasia
Ultrasound: can be done, but less specific than scintigraphy
PTH and Vitamin D levels
Biopsy
- A 68-year-old nonsmoking man has been complaining of progressive weakness for 2 weeks.
In addition to these symptoms he has developed intermittent cough, pleuritic chest pain and exertional dyspnea for 6 days. In the last weeks he frequently experienced nausea and vomited several times.
Medical history reveals no hypertension or coronary artery disease.
He has a long history of heartburn – he takes regularly antacids and drinks 1–2 L milk a day.
Laboratory findings:
serum Ca: 2.8 mmol/l
serum phosphate: 1.8 mmol/l
BUN: 24 mmol/l
HCO3-: 38 mmol/l
PTH and vitamin D: normal.
What is the most likely diagnosis?
Probable Diagnosis: Milk-Alkali Syndrome:
the chronic ingestion of high amount of antacids and milk + hypercalcemia are strong clues
Hypercalcemia: (normal 2.2-2.6 mmol/L)
- Ingestion of too much bicarbonate (and its negative charges) leads to corresponding absorbance of positively charged calcium
- Hypercalcemia can have a CNS-depressing effect, this leads to autonomic dysfunction that causes GI symptoms (nausea + vomiting) as well as explaining the progressive weakness the patient is experiencing
Hyperphosphatemia: (normal 0.8-1.45 mmol/L): sign of renal failure
High BUN: (normal 2-10 mmol/L)
- Chronic milk alkali syndrome leads to kidney failure via nephrocalcinosis
High bicarbonate: (normal 21-26 mmol/L)
- Over-absorption of bicarbonate causes the person to have mild alkalosis
Pleuritic chest pain, dyspnea, cough: hypercalcemia may have made ectopic calcifications of the lungs
PTH and Vitamin D normal: rules out other potential causes, like hyperparathyroidism
- A 35-year-old woman is complaining about frequent muscle cramps. She was admitted to the hospital after having a convulsion.(sudden movement of the body)
She had thyroidectomy 3 months ago and she is on thyroid hormone substitution since then.
Physical examination revealed a positive Chvostek’s sign and Trousseau’s phenomenon.
Laboratory findings:
serum Ca: 1 mmol/l
serum phosphate: 2.0 mmol/l
serum ALP 140 U/l
What is your diagnosis? What further test(s) would you order to support your diagnosis?
Diagnosis: PTH Deficiency due to Thyroidectomy where the parathyroid glands were also lost in the surgery
Severe hypocalcemia: (normal 2.2-2.6 mmol/L) - this is a life-threatening level; she is at risk of laryngeal spasm that could occlude her airway
Hypocalcemia causes hyperexcitability of the muscles, leading to symptoms of muscle cramping, convulsion,
Chvostek sign: touch the masseter muscle ⇨ twitching
Trousseau’s phenomenon: inflate blood pressure cuff ⇨ flexor muscles in hand and forearm contract/spasm.
(not to be confused for Trousseau’s other phenomenon: migratory thrombophlebitis)
Hyperphosphatemia: (normal 0.8-1.45 mmol/L)
- PTH normally stimulates phosphate excretion. Without PTH ⇨ serum [Pi] ↑
Normal ALP: ( < 150 U/L)
Further Tests:
PTH levels: see if there is any endogenous production left
Imaging: maybe do scintigraphy to see if there is any uptake
(May also check for vitamin D deficiency, since PTH stimulates vitamin D synthesis via 1-α OHase stimulation; PTH supplementation would probably fix this, so testing is not entirely necessary)
- A 66-year-old woman felt a sharp, sudden lumbar pain as she was lifting a bag of groceries out of the supermarket cart.
An X-ray taken in the emergency department showed a compression fracture of L1 vertebra.
Laboratory findings:
serum Ca: 2.4 mmol/l
serum phosphate: 1.1 mmol/l
What is your diagnosis? What further tests would you order?
Diagnosis: Pathological Fracture - fracture during normal activity, likely due to Primary(postmenopausal) Osteoporosis
This person is very likely to have osteoporosis based on pathological fracture + demographics of 66 year old woman (postmenopausal, primary osteoporosis)
Estrogen stimulates OPG production, and OPG decreases osteoclast activity.
After menopause, low estrogen ⇨ overactive osteoclasts ⇨ extensive bone remodeling / osteoporosis
Normocalcemia (2.2-2.6 mmol/L) and Normophosphatemia (0.8-1.45 mmol/L) are both typical of primary osteoporosis, and rule out other causes:
If she had osteomalacia, Ca and Pi would probably be low
If she had hyperparathyroidism, Ca would be high and Pi could be low or high, depending on the origin of hyperparathyroidism
Further tests:
DEXA: see her T score to diagnose osteoporosis
Possibly additional labs: PTH, ALP, urinary calcium and phosphate. All should be normal.
Maybe check estrogen levels
- A 60-year-old diabetic woman has been on hemodialysis for 15 years. She recently started to complain of cardiac pain.
She has no history of cardiac illness.
Physical examination reveals pale, grey-yellow colored skin, but nothing else remarkable.
Exercise electrocardiogram shows ST-T alterations.
Laboratory findings:
ALAT: 45 U / l
ASAT: 52 U / L
ALP 120 U / l
Serum creatinine: 180 mmol / l
Serum Ca: 2.1 mmol / l
serum phosphate: 2.8 mmol/l
serum PTH: elevated
What is the possible diagnosis?? What further tests would you perform?
Possible Diagnosis: Renal Failure with Secondary Hyperparathyroidism
Several Known Mechanisms:
- Damaged kidney cannot remove enough phosphate ⇨ hyperphosphatemia ⇨ Pi binds to free Ca2+ ⇨ free [Ca2+] ↓ ⇨ stimulation of PTH secretion
- Damaged kidney has poor enzymatic conversion of vitamin D (1α-hydroxylase) ⇨ low vitamin D ⇨ reduced Ca2+ absorption ⇨ hypocalcemia ⇨ stimulation of PTH secretion
- High Pi levels stimulate osteoclasts to secrete FGF-23 ⇨ vitamin D synthesis inhibited ⇨ reduced Ca2+ absorption ⇨ hypocalcemia ⇨ stimulation of PTH secretion (FGF-23 also more directly stimulates PTH secretion)
Normal ALAT (normal < 45 U/L) - liver is fine
Slightly elevated ASAT (normal < 45 U/L)
- ASAT is also present in organs like the kidneys and heart, and the increased ASAT here could be relevant to either of these
Normal ALP (normal < 150 U/L)
High serum creatinine (normal 40-130 µmol/L)
- Indicates low GFR, poor kidney function
Slightly low calcium (normal 2.2-2.6 mmol/L)
- Due to mechanisms described earlier
High phosphate (normal 0.8-1.45 mmol/L)
- Due to renal failure with decreased renal excretion of Pi. High Pi leads to decreased vitamin D synthesis and increased PTH secretion
Elevated PTH indicates hyperparathyroidism
Cardiac pain and ST-T changes
These two signs indicate problems with repolarization, probably due to insufficient oxygenation. There is probably some macroangiopathy/ atherosclerosis due to diabetes and secondary hyperparathyroidism. She is also anemic, which worsens oxygenation. (Thanks Fredrik)
Note also the patient is at risk for arrhythmias from electrolyte disturbances:
Hyperkalemia is a common problem with chronic renal failure,
- and has a strong risk for V-fib.
Hypocalcemia can also cause cardiac/ECG changes (in particular QT prolongation), but I doubt the calcium level here is low enough to have that effect.
- The main risk of long QT interval is Torsade de Pointes.
Paleness may be related to anemia due to decreased EPO production with chronic renal failure. Gray-yellow skin also can be the result of severe chronic kidney failure.
What further tests would you perform?
Should perform many tests due to complicated effects of kidney disease
Rule out AMI by cardiac enzymes: Troponin T, CKMB, LDH1.
Ultrasound and/or Scintigraphy with 99mTc. Imaging for parathyroid gland hyperplasia
Other serum electrolytes: especially K+, but also Na+ and Cl-
Vitamin D levels: probably low
Related kidney diagnostics: BUN, creatinine clearance, urine volume, etc.
Blood glucose level, check for glucosuria
In Renal osteodystrophy, involves hyperparathyroidism and loss of bone mass (overactivation of osteoclasts -> Ca2+ is reabsorbed and lost by the kidney)
Consider DEXA
Treatment: VitD + calcium supplements
Note that if a patient goes with an untreated secondary hyperparathyroidism for too long (several years) he/she can develop a tertiary hyperparathyroidism. This means development of autonomous PTH secretion (Tornóci called it adenoma) that stays high even after treatment is applied.
- A 65-year-old man complains of frequent urination and urinary retention. There is no macrosopic hematuria, urination is not painful. He complains of recurrent abdominal pain in the last weeks.
Laboratory findings:
serum Ca: 3.5 mmol/l
serum phosphate: 2 mmol/l
BUN: normal
What is the possible diagnosis? What further tests would you perform to support your diagnosis?
Possible Diagnosis: Prostate Carcinoma with Bone Metastases
Prostate cancer frequently metastasizes to the vertebrae, where it can form Osteolytic bone lesions that (rarely) cause hypercalcemia and hyperphosphatemia
Bone metastases are more commonly “blastic” (bone-forming), inducing a cycle in which increased PTH→ causes bone resorption from other sites while increased PTH1-R expression on metastatic cells stimulates their growth and subsequent nearby bone formation.
Our department likes to hear about the osteolytic lesions as the source of hypercalcemia, but this is not all there is to it, and to me this explanation is more interesting and complete… sorry. (Ben). YALLLA YA FALTSANNN
Urinary retention and frequent urination + older male + no bleeding + no pain on urination all suggest that the prostate is enlarged.
Severe hypercalcemia (normal 2.2-2.6 mmol/L) - this is an alarmingly high level; he is at risk for cardiac arrest/coma. In hypercalcemia, calcium ions block the NMJ sodium channels, making muscle cells less excitable.
- Recurrent abdominal pain symptoms could be related to hypercalcemia causing loss of tonicity of the bowels and constipation. Could also be a peptic ulcer.
Elevated phosphate levels: (normal 0.8-1.45 mmol/L)
- Like elevated calcium, this can occur from neoplastic bone lesions
Having both elevated calcium and elevated phosphate levels shows that kidney disease is not the source of his problem
Normal BUN: despite urinary retention, kidney function seems OK
Further tests:
Prostate evaluation:
digital-rectal,
biopsy,
PSA
(although not specific nor sensitive for diagnostics; according to Molnar it is the bound form of PSA that is measured)
Imaging of Metastases:
CT,
X-ray,
MRI
ALP: may be elevated with bone destruction
PTH: due to the above-mentioned mechanism; suppression of serum PTH levels may help limit growth of PTH1R+ metastases (again, this is extra)
- What laboratory tests would you perform in case of an upper respiratory inflammatory disease accompanied with fever?
Mention a few positive/negative acute phase proteins!
Obtain Specimen / Make Culture: see if it’s streptococcus, viral etc.
WBC count: Normal range: 4-10 G/L
- Can suggest if infection is bacterial (neutrophils ↑) or viral (lymphocytes ↑)
Erythrocyte Sedimentation Rate (ESR): normal is < 20 mm/hour.
Non-specific marker of inflammation.
- Usually increases during inflammation due to increased production of acute phase proteins like fibrinogen, which is a large molecule that causes erythrocytes to stick together better, increasing their rate of sedimentation.
- Women tend to have higher ESR due to lower hematocrit as a result of menstrual bleeding
Technically, ESR should be between 2 and 10 mm/hour for men, and 20 mm/hour for women, but this is not on the lab diagnostic values sheet.
ESR > 100 mm/hour is an indicator of sepsis, pneumonia, and plasmacytoma
CRP: normal range: 1-8 mg/L
- CRP is a positive acute phase protein, increasing 100-1000x in acute inflammation.
*Note that very slight elevations in CRP within diagnostic “normal range” (3-8 mg/L) are used to measure chronic inflammation, and they are strong indications of risk for heart attack or stroke. The 1-8 range is only for checking for acute inflammation.
Procalcitonin: increases in severe bacterial, fungal, and parasitic infections
More specific than CRP
Serum Protein Electrophoresis: during inflammation, normally see: Albumin ↓ while Gamma globulins ↑
(described as A/G ratio ↓, which is a value we have to remember. Normal: 1.25-2.5)
Gamma range ↑ with IgG, IgA, IgM increases depending on the phase/type of infection
Positive Acute Phase Proteins: levels increase during inflammation
CRP: binds some bacteria and induces the complement cascade
- *S**erum Amyloid A: similar function to CRP. In chronic inflammation, may misfold and ⇨
- *amyloidosis**
Fibrinogen: clumps bacteria together
Ceruloplasmin: scavenges oxygen radicals generated by leukocytes
Protease inhibitors: α1-antitrypsin, α2-macroglobulin
Haptoglobin: binds globin in plasma for recycling, inhibiting microbe iron uptake
Complement factors: opsonize, perform chemoattraction signaling, MAC
Hepcidin: prevents uptake of iron (in chronic inflammation, this high hepcidin level can cause anemia)
Negative Acute Phase Proteins: levels decrease during inflammation
Transferrin:
bacteria need iron to grow, and inhibiting transferrin deprives them of an iron source
Albumin:
decreases to save amino acids for positive APP production and to prevent hyperproteinemia
Normal plasma protein values:
Total protein: 60-80 g/L
Albumin: 35-50 g/L
A/G ratio: 1.25-2.5
CRP: 1-8 mg/L
- What is the significance of an elevated ESR?
Erythrocyte Sedimentation Rate (ESR) is traditionally measured in a thin Westergren tube (nowadays it’s automated). Blood is allowed to sit in the tube for one hour, and the red blood cells settle (“sediment”) at the bottom of the tube at a variable rate measured in mm/hour. Depends on many factors.
The red blood cells are negatively charged, which have a repelling effect on each other. This effect is called the “zeta potential,” and it normally slows down the rate at which erythrocytes sediment.
Causes of Elevated ESR:
Anemias: due to lack of red blood cells, the zeta potential is reduced, allowing erythrocytes to settle faster (Zeta Potential ↓ = ESR ↑)
Pregnancy: erythrocyte sedimentation rate increases during pregnancy due to an increase in fibrinogen and globulin levels; there is however a fall in the amount of albumin
Some malignancies: such as lymphoma or multiple myeloma
Hypoalbuminemia:
albumin is also negatively-charged, and its large presence in the serum contributes to the repellant effect of RBCs. Without albumin, there is a lower negative repellant effect, and so RBCs settle faster ⇨ ESR ↑
Hypoalbuminemia usually is the result of liver or kidney failure
Inflammation:
fibrinogen is produced in large quantities in inflammation, and fibrinogen is a large protein that helps RBCs to clump faster ⇨ ESR ↑
- Similar effect occurs from hypergammaglobulinemia
ESR is measured in millimeters of sedimented RBCs / hour.
Males: 2-10 mm/hour
Females: 2-20 mm/hour
Women are more likely to have higher ESR due to comparatively lower hematocrit due to menstrual bleeding. Same mechanism as anemia but not severe enough to be pathological
- What is the direction of change in the parameters below during respiratory acidosis? During
Actual HCO3- - directly measured bicarbonate of the blood sample
Generation:
aHCO3- is dependent on both metabolism and respiration. In respiratory acidosis (not breathing sufficiently) pCO2 increases, and due to Le Chatelier’s principle more HCO3- is formed.
CO2 + H2O ←→ H2CO3 ←→ HCO3- + H+ (shifts rightward)
Compensation:
Standard HCO3-
Generation:
stHCO3- is only dependent on metabolism, because the value is measured after equilibrating the sample to 40 mmHg pCO2. There is initially no metabolic change (compensation), and thus no change in the value.
Compensation:
However, after the increase in HCO3- reabsorption we can see an increase in stHCO3-.
—————————————————————————————————————————-
Base excess (BE)
Generation:
this value shows base deficit reflecting the metabolic side, and initially there is no change in the metabolic side.
Compensation:
as explained above there will be an increase of HCO3- (base) due to kidney compensation, thus BE will show a positive value (pos. = base excess/lack of acids).
Note that compensation by the kidney takes maybe 6-8 hours before working, and up to 3-5 days before maximal effect. This is because synthesis of channel proteins in the kidney is needed for the compensation.
- Traumatic shock (bleeding, crush). The acid-base parameters
During first hours
pH indicates acidemia (normal is 7.35-7.45)
HCO3- indicates of metabolic origin (normal is 24 mmol/L)
AG cannot be determined. Cannot calculate corrected HCO3- without AG.
pCO2 is low (normal 35-45 mmHg), but expected pCO2 = 18-22 mmHg according to Winter’s formula (below).
- pCO2 measured is within this range, thus compensation is normal.
- Winter’s formula is used to calculate the expected pCO2 in respiratory compensation of an acid-base disorder, and its results are sometimes approximated as pCO2 ≈ last 2 digits of pH: pCO2 = (1.5 x HCO3-) + 8 +/- 2
BB is low (normal 45-52 mmol/L) because bases in blood are used up as buffers.
BE is strongly negative (normal 0 +/- 2.5 mmol/L) - lack of base, excess of acids
Conclusion: Primary metabolic acidosis with normal respiratory compensation.
One day later
pH indicates acidemia
Both pCO2 & HCO3- indicates acidosis
Expected pCO2 = 25.5-29.5,
- pCO2 measured is higher than the expected value, thus there is a coexisting respiratory acidosis. >50 mmHg -> hyperkapnia.
No change in BB or st.HCO3- can indicate lack of kidney compensation? (just something I believe)[1] [2] [3] [4] [5]
Conclusion:
the original metabolic acidosis has worsened due to inadequate lung compensation because of ARDS (referred to as “shock lung” in the question).
- *Metabolic acidosis + respiratory acidosis**
