Cases semester 1 - random Flashcards
1
Q
- What tests would you perform if you suspect your patient has an autoimmune inflammatory bowel disease?
A
- If patient has not already reported visible blood in stool → hemoccult
- Colonoscopy/endoscopy with biopsy - always done for suspected UC or Crohn’s
- If nothing is found via colonoscopy/endoscopy, can perform capsule endoscopy
- Stool culture + microscopy to rule out microbial/helminthic infection
- Systemic inflammatory markers such as CRP or ESR
- Antibodies can be tested such as ASCA (anti-S. cerevisiae, common in Crohn’s) and p-ANCA (common in UC)
(**Chron’s / Colitis ulcerosa (diagnosis: endoscopy [biopsy: histologically they are very different])Chron’s - transmural | Colitis ulcerosa - only mucosaChron’s - inf. anywhere |. (ileitis terminalis)| Colitis ulcerosa - Rectum/**)
2
Q
- A middle-aged man saw his family doctor, because he got rashes. On examination he was
found to have extensive yellowish papules, with an erythematous base, on his buttocks and
elbows and orange-yellow discoloration of the palmar creases.
Fasting lipids: serum cholesterol 7.6 mmol/l, triglyceride 8.1 mmol/l.
What is your diagnosis?
A
- High serum cholesterol (>5.2 mM) and very high TGs (>1.7 mM).
- Discolored palmar crease = xanthoma striatum palmare
- Lipid increase pattern + xanthomas indicative of familial type III hyperlipoproteinemia
- due to an autosomal recessive Apo E mutation (a defective “ApoE2” form)
- results in increased TGs and IDL
- also known as “familial dysbetalipoproteinemia” or “remnant hyperlipidemia” because of Apo E’s role in removal of VLDL remnants (IDL)
- Can test for the mutated gene, must have two mutated alleles.
- Xanthomas + atherosclerosis develop due to increased accumulation of cholesterol within scavenging macrophages
(**Hyperlipidemia type III**)
3
Q
- A patient with symptoms of chronic alcoholism complains of recurrent abdominal pain, meteorism. He has lost weight in the past few months, his stools are voluminous, difficult to flush.
- serum Ca: 2.1 mmol/l
- prothrombin time INR: 2.6; normalized after vitamin K administration
- serum glucose (fasting): 12 mmol/l
- ALP: 264 U/l
- albumin: 40 g/l
- fecal elastase: decrease
- dabdominal ultrasound: enlarged pancreas
What is your diagnosis? What other tests would you do?
A
- Probably chronic pancreatitis because of normal albumin (would be lowered in acute phase rxn).
- Main cause of this is alcoholism , but may also be autoimmune.
- “Meteorism” (bloating) and big, difficult to flush stool → issues digesting fat → steatorrhea
- Slightly low serum Ca++ (<2.2 mmol/l) via two mechanisms:
- decreased vitamin D absorption via fat malabsorption
- “saponification” of FFAs with Ca ++ in the damaged pancreas
- Prothrombin time elongated (>1.2 INR) fixed by vit. K → fat/vit. k malabsorption
- Very high fasting glucose (>7 mmol/l) → decreased insulin production
- High ALP (>150 U/l) → bone resorption to accommodate ↓ Ca ++
- Hamar: ALP increase here is mild, so obstruction is not the likely cause of pancreatitis.
- Enlarged pancreas on US → pancreatitis
- Normal albumin (35-50 g/l) → inflammation is not acute
- Fecal elastase decrease → decreased pancreatic exocrine activity
- Elastase is synthesized equimolar with other pancreatic enzymes + its level in fecesindicates exocrine activity (decrease indicates chronic pancreatitis)
- Need to rule out pancreatic cancer so must perform Endoscopic retrograde cholangiopancreatography (ERCP)
(**meteorism - a lot …Chronic pancreatitisLack of lipase - lipid digestion -> Mal absorption of lipids -> Mal absorption of vit KDiabetes may develop ..Elastase - produced in the pancreas (many others are digested)Ca++. a bit lower - vit K is lower, we can assume that Vit D is also low (bone…)IV secretin - chole… than sucking the produced pancreatic juice (disadvantage - tube is needed)Pancreolauryl test**)
4
Q
- A young girl develops virilization and hypertension . Plasma cortisol is low, ACTH is elevated.
What is the most likely cause of this condition?
How are adrenal production of glucocorticoids, mineralocorticoids and androgens affected?
A
- Virilization with low cortisol suggests adrenogenital syndrome, a form of congenital adrenal hyperplasia (CAH).
- This is most commonly due to an autosomal recessive 21-OHase deficiency, leading decreased mineralocorticoid/glucocorticoid and increased androgen production.
- Excess androgens cause virilization, hirsutism, infertility and premature adrenarche.
- Lack of aldosterone leads to hyperkalemia and hypotension.
- (Since this patient is hyper- rather than hypotensive, this is a different enzyme deficiency.)
-
Lack of 11β-hydroxylase, another autosomal recessive disorder, is a much more rare form of CAH (only 5%).
- Androgen excess causes the same symptoms as in 21-OHase deficiency.
- 11-Deoxycorticosterone (DOC) , an aldosterone precursor with mineralocorticoid activity, accumulates and can lead to hypertension and hypokalemia.
- Since this patient was hypertensive it is most likely the rarer 11β-hydroxylase form of adrenogenital syndrome.
- Treatment is cortisol supplementation to suppress ACTH and thus androgen/MC excess (as well as replacing the lacking cortisol).
5
Q
- A 30 year-old man complains of recurrent abdominal pain usually accompanied with diarrhea. These symptoms occur after the ingestion of fresh dairy products or alcohol.
What may be the cause of these complaints? What tests would you do?
A
- This is lactose intolerance which can be worsened by alcohol, because it decreases lactase activity.
- Tests :
- Lactose Hydrogen Breath Test - patient swallows a lactose solution and their breath is checked every 20-30 mins for 2-3 hours against a baseline measurement for large increases in hydrogen gas
- Blood Glucose Test - lactose malabsorbers will generally see less of an increase inblood glucose after ingesting lactose
- Stool Acidity Test - for infants b/c they don’t cooperate with
(**Lactose intolerance(HBT)Alcohol - inhibits enzyme activity (worsen the symptoms)**)
6
Q
- An 11 month old baby with protruded belly and retarded in movement development has been brought for medical evaluation. Serum FT4 and FT3 are decreased. Serum MIT/DIT are elevated and their urinary excretion increased. What is the most likely diagnosis?
A
- Cretinism - severely stunted mental/physical development due to congenital thyroid hormone deficiency.
- Cretinism can be due to “endemic” causes such as iodine deficiency, or genetic causes leading to enzyme or other protein deficiencies.
- Since MIT/DIT are elevated, but FT3/4 are decreased, this is likely a TPO deficiency resulting in an inability to sufficiently iodinate thyroid hormones. (Says Tunde, but I can’t read about this anywhere else.)
- Other genes/proteins altered in congenital hypothyroidism are TSH-R , TG , and iodotyrosine deiodinase.
- Perchlorate Test - Perchlorate is a competitive inhibitor of thyroid iodine uptake. First, administer radiolabeled iodine and perform scintigraphic measurement. Then administer perchlorate and re-measure scintigraphy. If TPO is functional, the “warmth” of the picture remains stable because much of the iodine has been oxidized and incorporated into hormones; if TPO is dysfunctional, perchlorate’s blocking of new iodine entry into the gland decreases the “warmth” of the image.
7
Q
- A 38 year-old woman complains of recurrent, sharp pain in the right upper quadrant of her abdomen. She has been vomiting , has fever and jaundice .
Laboratory results:
- serum bilirubin: 50 μmol/l, mostly direct
- Ubg: negative
- ASAT: 180 U/l
- alkaline phosphatase: 640 U/l
What is the cause of her symptoms, and how can you prove the diagnosis?
A
cholelithiasis
- Sharp RUQ pain indicate possible gallstones
- High, mostly direct bilirubin (>17 umol/l) indicates obstructive jaundice
- ALP elevation (>150 U/l) indicates obstruction
- Negative Ubg also indicates obstructive jaundice (no bilirubin → GI tract)
- ASAT elevation (>45 U/l) indicates liver damage
- Vomiting and fever indicate possible cholecystitis
- Prove the possibility of cholelithiasis with abdominal ultrasound.
8
Q
- A hypertensive male patient enters the hospital for medical evaluation. His blood pressure is 180/95 mmHg ; Serum Na+: 148 mmol/l, K+: 3.5 mmol/l, fasting plasma glucose: 7.2 mmol/l. Baseline plasma cortisol was elevated. A small dose of dexamethasone did not suppress cortisol. A large dose of dexamethasone was given but there was little change in the blood cortisol from baseline values. Plasma ACTH was high. What is the most likely diagnosis?
A
- Since ACTH was high and both low/high dose dexa tests produced no change, this is ectopic ACTH syndrome
- Hypertension, hypernatremia and hypokalemia (K+ actually at low end of normal in this case) can be explained by the fact that cortisol has mineralocorticoid activity and thus may produce similar effects to hyperaldosteronism. This effect is especially common in ectopic ACTH syndrome.
- Glucose is elevated due to cortisol’s gluconeogenic effects.
- A chest/abdomen CT should be performed and any ectopic ACTH source removed.
9
Q
- A newborn baby is admitted to the hospital with a complaint of increasing jaundice. The serum bilirubin is 160 μmol/l.
What can be the cause of the jaundice if this bilirubin is mainly:
- direct, or
- indirect reacting?
A
-
Causes of direct hyperbilirubinemia:
- Infection - hepatitis or any other infection can ↓ liver function
- Biliary atresia - improper development of bile ducts
- Dubin-Johnson Syndrome - AR mutation of canalicular MRP2 → ↓ hepatic excretion of bilirubin glucuronide (liver appears black)
- Rotor Syndrome - AR mutation of OATP1B (organic anion transporting polypeptide) proteins for hepatic uptake of of bilirubin
-
Causes of indirect hyperbilirubinemia:
- Physiological jaundice - before birth glucuronyltransferase is downregulated in the fetus to keep bilirubin unconjugated and thus able to pass through the placenta and not accumulate in the fetus; it takes some time to fully function after birth b
- Erythroblastosis fetalis - via Rh incompatibility → hemolysis
- Gilbert’s Disease - low UDP-g transferase function, often asymptomatic unless stressed
-
Crigler-Najjar - 2 types: total or partial lack of UDP-glucuronosyl transferase
- severe form can lead to kernicterus (bilirubin in brain) → brain damage
- only treatment is liver transplant
- phenobarbital can induce the enzyme in the less severe form
- severe form can lead to kernicterus (bilirubin in brain) → brain damage
- Phototherapy can be used to solubilize excess dermal bilirubin in neonatal jaundice.
10
Q
- A diabetic man treated with insulin skipped his late evening meal before going to bed,without any change in his insulin administration. He has been sweating a lot during the night, and glucose has been detected in his urine in the morning.
What is the explanation for this?
A
- Paradox/Somogyi Effect - no meal + insulin = hypoglycemia → sympathetic activation → sweating + ↑ insulin antagonist hormones (cortisol/glucagon/GH/catecholamines/T3/T4) → gluconeogenesis → hyperglycemia + morning glucosuria
- treatment is actually carb intake and/or less insulin administration
- (not sure about that part… that’s what Tunde said… i guess carbs → ↓ insulin antagonists/gluconeogenesis and then ↓ blood sugar? but seems weird … also Wikipedia says the Somogyi effect might be fake…)
11
Q
- A patient complains of intense periumbilical pain of sudden onset. His blood pressure is low, the pulse is fast, he is sweating and has nausea. There is no defense on physical examination of the abdomen.
Laboratory results:
- ESR: 42 mm/h
- WBC: 11 G/l
- serum α-amylase: 1800 U/l
- urine α-amylase: increased
- serum lipase: increased
- serum urea: 10 mmol/l
- serum creatinine: 90 μmol/l
- serum Ca: 1.9 mmol/l
- serum albumin: 30 g/l
- fasting blood glucose: 6.5 mmol/l.
What is your diagnosis? What other tests would you perform?
A
- High α-amylase (>180 U/l), urine amylase and serum lipase indicates pancreatitis
- Periumbilical or “belt-like” pain is typical of pancreatitis.
- This is acute pancreatitis , because of the high ESR, low albumin and high serum/urine pancreaticenzymes.
- High ESR (>20 mm/h) → inflammation
- In inflammation, increased serum fibrinogen causes RBCs to stick together and form”rouleaux” which settle faster via increased density.
- High WBC (>10 G/l) indicates inflammation / immune reaction
- Serum albumin is low (<35 g/l) indicating acute inflammation
- Fasting glucose is high (>6.0 mM) → low insulin secretion, but not actually…
- ~90% islets must be destroyed before glucose ↑
- in acute inflammation, stress hormone elevation → high gluconeogenesis
- Low BP + tachycardia point to the beginnings of shock.
- Shock Index = HR / Systolic BP … should be around 0.5-0.66 … >1 indicates probable shock (means ↑ HR ↓ BP)
- Serum urea is borderline high → slightly impaired kidney function
- can be via redistribution of blood flow in early shock (low BP, high HR)
- Creatinine is normal (40-130 uM)
- Ca++ is low (<2.2 mM) indicating impaired fat digestion → ↓ vitamin D
- In pancreatitis, autodigestion via lipase → “saponification” of FFAs + Ca → ↓ Ca++ (elongated QT on ECG)
-
Commonly caused by cholelithiasis or alcohol and greasy foods.
- Alcohol dehydrates pancreatic secretions + need for more lipase to digest foods → viscous secretions back up in pancreatic ducts → autolysis + inflammation
- Imaging studies (US, CT or MRI) can be done to confirm pancreatic enlargement
- Treatment is symptomatic: NPO (“nil per os”, no food/drink by mouth) and painkillers
12
Q
- A 47 year-old man has been on hemodialysis for 5 years before he got his kidney transplantation . He has little body hair , a large, protruding belly , slim extremities and gynecomastia.
Laboratory results:
- ASAT: 85 U/l
- ALAT: 76 U/l
- prothrombin time: INR = 2.7; it does not change after vitamin K administration
- albumin: 28 g/l
- K+: 3.3 mmol/l
- Ht: 0.36
What is the most likely diagnosis?
A
- This is most likely cirrhosis via a chronic iatrogenic hepatitis from dialysis.
- Blood transfusions are common after dialysis, and can lead to hepatitis C infection (according to Hamar).
- dialysis is a risk factor for iatrogenic hepatitis
- equally, but not extremely elevated ASAT/ALAT (>45 U/l) indicate chronic non-alcoholic liver damage
- elongated PTR (1.2 INR) unresponsive to vit. K indicates liver damage → coag. factor deficiency
- decreased albumin (< 35 g/l) indicates liver dysfunction
- low K + (<3.5 mM) probably via:
- ascites (“protruding belly”) → ↓ circulating fluid volume → activation of RAAS in kidney → ↑ aldosterone → ↑ K + excretion
- “effeminate” body constitution (↓ hair, breasts, slim limbs) indicates liver dysfunction
13
Q
- Plasma cortisol level of a patient is lower than normal. Urinary aldosterone excretion is decreased and the patient is hypoglycemic. What is the most likely diagnosis and what tests would you order?
A
- Deficiency of both cortisol and aldosterone indicate primary adrenal insufficiency which has several possible causes:
- Autoimmune - **Addison’s** (often against 21-OHase), Autoimmune polyendocrine syndrome (affects multiple endocrine glands)
- Infection - as in meningococcal Waterhouse-Friderichsen syndrome , tuberculosis (adrenal insuffic. is often 1st sign of TB), pseudomonas, fungi or viruses
- Congenital Adrenal Hyperplasia - usually via 21-OHase genetic defect
- If the onset was rapid, or any other signs such as petechial rash are present, suspect meningococcal infection.
- CSF microscopy to check for presence of gram negative diplococci either in the fluid or in WBCs; PCR can also be used if available
- If onset was slower, suspect Addison’s disease.
- ACTH stimulation test - uses synthetic ACTH “tetracosactide”; short (small dose, test cortisol 1 hr later) and long (large dose, test cortisol 4 times over 1 day) versions are done; if appropriate cortisol response is seen, Addison’s can be ruled out
- Other signs of Addison’s are ↑ Ca ++ / ↓ Na + / ↑ K + / metabolic acidosis / ↑ WBCs (but none of these are specific)
- Skin bronzing is another sign of Addison’s. Can check the gums/oral mucosa for bronzing in places with no sun exposure.
- If Addison’s is present, hormone therapy is needed
- Note: the hypoglycemia is due to loss of cortisol’s gluconeogenic effects.
14
Q
- A 45 year old patient complains of maldigestion, increasing abdominal pain and weakness. Abdominal discomfort occurs shortly after meals or alcohol ingestion. Laboratory results:
- Haemoccult: +
- anemia
What tests would you do, what are the treatment options?
A
- Positive hemoccult and anemia in 45 yr. old w/ abd. pain → maybe malignancy, but…
- Pain shortly after meals/alcohol → peptic ulcer is mostly likely
- May also be IBD (Crohn’s / UC)
- Tests :
- Endoscopy + biopsy to check for presence of ulcer and culture it for H. pylori and alsoto differentiate between ulcer and cancer
- Urea Breath Test - isotope-labelled urea solution is swallowed, if H. pylori is present, itsurease breaks down urea into isotope-labelled CO 2 which is detected in patient’s breath
- If the above tests are negative for ulcer / H. pylori, use the tests mentioned in the next question for IBD.
- Treatment :
- If H. pylori positive → triple therapy : clarithromycin, amoxicillin and PPI
(**Abdominal discomfort occurs shortly after meals - typical for … (ulcer)Haemoccult: + (peptic ulcer have a tendency to bleedother: gastroscopy+biopsy (h.pylori, gastric cancer biopsy)Differential: - Drugs NSAID - ….**)
15
Q
- The laboratory parameters of a male person having normal blood pressure, BMI 23 kg/m2 are:
- serum TG: 1.5 mmol/l
- serum LDL cholesterol:4.4 mmol/l
- serum CRP: 5 mg/l
What is the risk of CHD for this person? What are the risk factors of atherosclerosis?
A
- TGs and BMI are normal
- LDL is high (>3.4 mmol/l)
- CRP is within normal range, but still above the 3.0 mg/L cut-off for high risk of CHD development
- Because of higher CRP and high LDL, patient is at high risk for developing CHD.
- Atherosclerosis Risk Factors:
- Non-modifiable: age, sex, genetics
- Modifiable: smoking, exercise, hypertension, weight, diet, stress
16
Q
- Laboratory data of a patient with arterial hypertension include increased Na+ and decreased K+ concentrations. Urinary aldosterone excretion is twice normal. What is the most likely diagnosis if plasma renin activity is 1) high 2) low?
A
- With high renin, some kind of kidney dysfunction or primary hypersecretion of renin is likely. There are two likely possibilities:
- Renin-secreting tumor - these are rare, can perform imaging studies to check for this.
- Low RBF (renal blood flow) - this could be due to blood or plasma loss, but the question mentions hypertension, so that is unlikely; external compression of the renal artery by a tumor or internal occlusion of the renal vessels by thrombosis/embolism are possible
- CHD - Congestive heart failure
- With low renin, some form of primary hyperaldosteronism -Conn’s syndrome-
is present. This has two common causes:- Bilateral idiopathic adrenal hyperplasia - 66% of cases, usually due to a congenital adrenal enzyme defects
- Adrenal adenoma - 33% of cases, can lead to hypertension, muscle issues and cardiovascular issues due to ion imbalances
17
Q
- A patient with apparent symptoms of hypothyroidism. What laboratory tests would be the most appropriate to perform?
A
- TSH - measured first and if normal, problem is likely not in the thyroid, because negative feedback mechanisms usually alter TSH levels in case of hyper-/hypothyroidism.
- if TSH high and T3/T4 low - primary hypothyroidism , check antibodies:
- anti-TPO antibody - in most Hashimoto’s and Graves’ patients
- anti-TSH-R antibody - stimulating form in all Graves’ and “blocking” form in some Hashimoto’s and later-stage Graves’ patients
- anti-TG antibody - in most Hashimoto’s and some Graves’ (30%)
- if TSH low and T3/T4 low - secondary hypothyroidism:
- administer TRH: if it doesn’t help, the problem is in the pituitary; if it does, the problem is hypothalamic (“tertiary hypofunction”, very rare)
- Hypothyroid symptoms :
- fatigue, feeling cold, constipation, depression, weight gain, hair loss
- myxedema - ↑ TSH stimulates fibroblasts to deposit more glycosaminoglycans → osmotic edema
- hoarse voice, poor memory/concentration
- ascites, pleural/pericardial effusion
(**fT3; fT4 to check for hypfunction look for the reason If TSH is low - secondary; tertiary (TRH stimulation test is needed)**)
18
Q
- A 25 year-old man has been icteric for a few days.
His laboratory values:
- serum indirect bilirubin: 47 μmol/l
- serum direct bilirubin: 4 μmol/l
- ASAT: 18 U/l ALAT: 23 U/l
- alkaline phosphatase: 66 U/l
- Ht: 0.48
- Hb: 162 g/l
What is the cause of his jaundice?
What further tests are necessary?
A
- This is Gilbert syndrome , slightly decreased UDP-g transferase activity. Only slightly increased indirect bilirubin is seen, with no other abnormal findings.
- Indirect bilirubin increase with normal direct indicates indirect hyperbilirubinemia (conjugation enzyme issue)
- Normal ASAT/ALAT/ALP indicate no liver damage/obstruction
- Normal Ht/Hb (>0.4 l/l and >135 g/l) indicates no hemolysis
- Test : No further tests are necessary, but Tunde says you can do this (if you hate your patient):
- Have the patient fast (<1000 kcal/day) for 2 days and then measure indirect bilirubin. If it has doubled from your initial measurement, this confirms Gilbert’s syndrome.
- (Acute stress can cause otherwise “silent” Gilbert’s to show symptoms. This test simulates that effect.)
19
Q
- A schoolgirl at the age of 14 without any complaints develops diffusely enlarged painless thyroid glands recognized accidentally by the school doctor. Laboratory findings: FT4 is slightly decreased , whereas total T3 is slightly elevated. Thyroid uptake of radioiodine is increased. FT4 gets normalized after treatment with inorganic iodine. What is the most likely diagnosis? Try to interpret the opposite changes in hormone levels.
A
- Enlarged, painless thyroid gland → goiter
- Since inorganic iodine normalizes T4 → iodine deficiency is the likely cause.
- Endemic goiter is the term for this, in reference to the fact that it is often endemic in areas with soil (and thus food) of low iodine content. Iodine deficiency is rare in developed countries now, but may occur in pregnancy and puberty .
- Radioiodine uptake is increased. The Na-I symporter (NIS) is regulated in two ways, both of which may be at play here:
- Plasma iodide - an increase will downregulate NIS, a deficiency will upregulate it
- TSH - upregulates NIS transcription (TSH may be ↑ here due to low FT4)
- Because T4 incorporates 4 iodine atoms, whereas T3 incorporates only 3 and is more hormonally potent, T3 is preferentially synthesized in case of iodine deficiency .
20
Q
- A 40-year-old man complains of spells of headache , profuse perspiration (diaphoresis), nausea and palpitations. Arterial blood pressure is markedly elevated . Urinary VMA excretion is increased.
What is the most likely diagnosis?
What test would you order to confirm your diagnosis?
A
- This is probably pheochromocytoma, a norepinephrine-secreting tumor formed by chromaffin cells of the adrenal medulla.
- Sometimes known as “10% tumors” because ~10% of them are bilateral, extra-adrenal, familial or malignant.
- Extra-adrenal PCC-like tumors are called “paragangliomas”.
- All symptoms can be explained by increased adrenergic receptor stimulation.
- Vanillylmandelic acid (VMA) is a breakdown product of catecholamines.
- Tests:
- Urinary Homovanillic acid (HVA) can be tested to see if there is any dopaminergic excess involved.
- Serum Chromogranin A can be tested. It is a peptide related to neuroendocrine secretion and elevated in pheochromocytoma.
- Clonidine Suppression Test - clonidine is an adrenergic agonist which will normally decrease circulating catecholamines; in case of pheochromocytoma, no decrease is seen; requires careful monitoring and is not often used anymore
-
Imaging - ultrasound, MRI or CT of the adrenal gland
- 131 I-MIBG - a radiolabeled, adrenal-specific agent that can be injected to visualize the adrenal gland and any tumors that may be present within it
21
Q
- A 51-year-old man seeks evaluation for blurring of vision and headache. He has coarse facial features and enlarged extremities. The determination of which hormone would be the most straightforward in the patient? What other diagnostic procedure(s) would you order? (+treatment)
A
- IGF-1 is the hormone to check, because GH secretion is pulsatile and thus hard to measure accurately.
- Blurring of vision / headache → probably a GH-secreting adenoma compressing the optic chiasm and increasing pressure in the sella turcica.
-
Coarse facial features and enlarged extremities indicate acromegaly , which is caused by ↑ GH.
—————————————————————— - Can perform a GH suppression test:
- Normally insulin → ↓ glucose → ↑ GH
- In this test we administer glucose and, in a healthy patient, see a drop in GH.
- In patients with inappropriate GH secretion we may see less of a drop, no drop or a paradoxical increase.
- MRI can be done to verify the presence of an adenoma.
- Other pituitary hormones should be checked to assess the “mass effect” of the adenoma on the rest of the pituitary gland.
- Check visual field for possibility of bilateral hemianopsia.
—————————————————————— - Treatment: can include surgical removal of the tumor, dopamine agonists (bromocriptine/cabergoline) or somatostatin analogues (octreotide) to ↓ GH secretion, GH-R antagonists or radiation (if surgery can not remove entire mass)
22
Q
- A 28 year-old woman. She is complaining of fatigue, malaise and nausea.
- serum total bilirubin: 45 μmol/l
- ALAT: 220 U/l
- alkaline phosphatase: 200 U/l
- γ-globulins: 33 g/l (↑)
- RF and ANA: positive
What is the most likely diagnosis, and what tests should be done?
A
- This is most likely systemic lupus erythematosus causing an autoimmune hepatitis. (AIH1)
- Increased total bilirubin (>17 umol/l) → hyperbilirubinemia
- Elevated ALAT/ALP (>45 U/l) → liver damage, possibly obstructive
- Some complaints could be due to pregnancy (fatigue, malaise, nausea) and ALP is increased in pregnancy. A more specific test for liver damage would be GGT .
- RF/ANA → SLE
- γ-globulin increase indicates excess circulating antibodies
- Check other antibodies: anti-Smith antigen (RNA-binding protein) and anti-cardiolipin
- It is possible, but rare, for Hep B/C to induce the formation of RF/ANA, so must rule these out.
23
Q
- A patient with Cushing’s syndrome entered the hospital for diagnostic studies. Baseline plasma cortisol was elevated. A small dose of dexamethasone did not suppress cortisol but 50% reduction occurred when large dose of dexamethasone was given. Plasma ACTH was elevated. What is the most likely diagnosis?
A
- Cushing’s syndrome is a collection of signs/symptoms related to excess cortisol exposure.
- due to excess exogenous corticosteroid (i.e. prednisone)
or a corticosteroid/ACTH-secreting tumor.
(These tumors can be within the pituitary/adrenal gland or ectopic.)
- *————————————————————————–**
- Cushing’s disease is a cause of Cushing’s syndrome involving increased ACTH secretion usually either via pituitary adenoma or elevated hypothalamic CRH secretion. **It does not include ectopic (non-pituitary) ACTH secretion.
- ————————————————————————-**
- Dexamethasone is a synthetic corticosteroid that provides negative feedback on the pituitary in order to decrease ACTH secretion.
- *————————————————————————–**
- Dexamethasone Suppression Test - uses both low (2 mg) and high (8 mg) doses to determine presence and cause of Cushing’s syndrome after a 24-hr urinary free cortisol test determines elevated cortisol
- Low-Dose (2 mg) - if cortisol is suppressed, no endogenous cortisol hypersecretion exists (i.e. no Cushing’s syndrome);
if it is not suppressed, some form of Cushing’s syndrome exists → ACTH levels must be checked and then high dose test is performed to determine the cause.
- *————————————————————————–**
-
High-Dose (8 mg) - several possible reactions exist:
- Low ACTH / No Cortisol Suppression - ACTH-independent Cushing’s syndrome
- AKA “adrenal Cushing’s”, either adrenal hyperplasia or neoplasm is likely
- perform adrenal CT and adrenalectomy if necessary
- Normal or High ACTH / No Suppression - ectopic ACTH syndrome
- often via a small cell carcinoma of lung
- perform chest/abdominal CT and surgical removal of ectopic source
- Normal or High ACTH / Suppression - pituitary Cushing’s disease
- an ACTH-secreting pituitary adenoma is likely
- pituitary adenoma = most common cause of Cushing’s syndrome (90%)
- Low ACTH / No Cortisol Suppression - ACTH-independent Cushing’s syndrome
-
High-Dose (8 mg) - several possible reactions exist:
perform pituitary MRI and hypophysectomy if necessary
————————————————————————–
- If the high-dose result is unclear, a CRH-stimulation test can be done via administration of IV CRH, and inferior petrosal sinus sampling is done to determine the source of elevated ACTH.
- If CRH raises petrosal sinus ACTH levels → pituitary Cushing’s disease
- If CRH does not raise ACTH levels → ectopic ACTH
- In this case, since ACTH levels were high, and high dose dexa suppressed cortisol levels, the patient most likely has Cushing’s disease involving a pituitary adenoma.
- A pituitary MRI should be performed.
24
Q
- A 15-year-old girl has been losing weight in spite of having a good appetite , and she feels tired lately. She has been admitted to a hospital for vomiting , being dizzy and disoriented.
- Laboratory findings:
- urine glucose: strongly positive
- ketone bodies: positive
- blood glucose: 28.5 mmol/l
- blood pH: 7.1
- serum K+: 5.4 mmol/l
What is your diagnosis, and what is to be done with her?
A
- Current condition: Diabetic ketoacidosis , as indicated by the blood + urine glucose (diabetic), ketone bodies (keto-) and low PH/high K + (-acidosis!).
- Underlying cause: Type 1 Diabetes Mellitus , as indicated by the patient’s age, weight loss (rather than gain seen in type 2), and blood/urine glucose (> 11 mM random blood glucose indicates DM without need for further testing). Type 1 can be confirmed by checking for islet cell/insulin/glutamic acid decarboxylase autoantibodies
.————————————————————————- - Symptom explanations:
- tiredness due to “fasting” cells (no insulin to stimulate glucose uptake)
- weight loss due t_o use of muscle protein & TAG (glycerol) from adipose tissue_ for gluconeogenesis
- dizziness/disorientation via dehydration (glucose → osmotic diuresis)
- nausea via acidosis → vomiting helps excrete acid
-
Hyperkalemia occurs because: ↓ glucose in cells → ↓ Na/K-ATPase activity → ↑ EC K + and metabolic acidosis → renal H + excretion → renal K + reabsorption
.————————————————————————- - Treatment: IV fluids and insulin (2-3 units/hr), both slowly to avoid complications
- GLUT2/3 transport in neurons can become dysfunctional with fast ↓ glucose so a 5 mM/day reduction is best
- cerebral edema can occur with fast ↑ fluids
- pH monitoring and K+ monitoring is important, as there may be a hypokalemic rebound when Na/K-ATPases begin to function again, requiring K + infusion
- older T1DM patient may require bicarbonate for pH normalization
31
Q
- After finding high lipid concentrations in the serum, what tests would you employ to confirm or exclude the secondary causes of hyperlipidemia?
A
ODACHECHGK
-
Obesity/Metabolic Syndrome - more FFA → more liver TAGs → ↑ VLDL → ↑ LDL ↓ HDL
- measure waist circumference, BMI, fasting glucose, BP, TAGs + HDL
-
DM - ketone/FFA efflux from adipose → liver TAGs + VLDL → ↑ LDL / ↓ HDL
- perform the WHO diagnostic algorithm (random glucose → fasting glucose → OGTT)
- type I pt only develops dyslipidemia if untreated; type II usually has dyslipidemia
- in type II, LPL activity ↓ so chylomicrons + VLDL ↑
-
Alcoholism - ↓ NAD + → ↓ β-oxidation → ↑ TAG synthesis
- measure GGT
- moderate alcohol intake inhibits CETP → ↑ HDL
-
Cushing - ↑ glucocorticoids → ↑ VLDL synthesis → ↑ serum LDL (mild)
- measure serum cortisol
-
Hypothyroidism - synthesis + activity of LDL-R ↓ → serum IDL/LDL ↑
- check TSH, T3, T4
-
Estrogen Treatment/Pregnancy - ↑ VLDL synth and ↓ hepatic lipase activity → ↑ TG/Chol.
- should only be treated with diet
- Cholestasis - see ↑ “Lipoprotein X” (LP-X) an abnormal low density lipoprotein
-
Hepatic Disease - primary biliary cirrhosis + obstructive liver diseases → ↑ cholesterol
- ASAT, ALAT, albumin and GGT can be measured
- LP-X also seen
- Glycogen Storage Disease - ↓ G-6-phosphatase (von Gierke) → adipose FFA efflux ↑ → TAG synthesis ↑
-
Kidney Disease - proteinuria → hypoalbuminemia → ↑ protein synth (thus apoproteins) → lipids ↑
- measure albumin, protein content of urine
- in kidney transplant, immunosuppression glucocorticoids → ↑ lipids
