Dx of ADR and Case Studies Flashcards

1
Q

Causes of ADRs

A
  1. Inherent drug characteristics (API, excipients)
  2. Quality problems (Contamination, substandard, counterfeits)
  3. Adulteration (potent API/analogues)
  4. Substitution of Ingredients
  5. DDI, D-food interactions
  6. Long term exposure/high dose
  7. Individual susceptibility
  8. In-use issues like non-adherence
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2
Q

What are some occurrences that most likely signify a drug association

A
  1. SJS
  2. TEN
  3. Agranulocytosis
  4. Acute Dystonias
  5. DILI (if other causes excluded)
  6. Cushing’s syndrome (if endogenous causes excluded)
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3
Q

How is ADR diagnosed?

A

When possible causes are excluded

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4
Q

Distinguish between SJS and TEN

A

Use percentage epidermal detachment of total BSA

  • SJS: <10%
  • TEN > 30%
  • Transitional SJS-TEN: 10-30%
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5
Q

Most common ADR of drug that causes withdrawal worldwide?

A

DILI

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6
Q

What do Dx of DILI include (repeated from PV deck)

A
  1. Hx of ingestion of drug (incl. CAM) within 12 months of onset of illness
  2. Exclude viral causes
  3. Exclude autoimmune
  4. Daily alcohol intake <20g
  5. Absence of biliary/focal liver pathology on ultrasound/CT scan of abdomen
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7
Q

Causes of Cushing Syndrome to exclude to confirm drug induced cushing syndrome?

A
  1. Adrenal Tumour
  2. Cushing Disease (too much ACTH)
  3. Ectopic ACTH-producing tumour (e.g. lung tumour)
  4. Exogenous source (e.g. unknown injection)
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8
Q

Toxic Heavy Metals Limit for Complementary Medicines

A
  1. As 5ppm
  2. Cd 0.3ppm
  3. Pb 10ppm
  4. Hg 0.5ppm
  5. Cu: Removed from list
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9
Q

What is the MoA of Mercury, and what is its adverse effects?

A

Inhibits formation of melanin by competing with Cu in action of tyrosinase enzyme. Forms inorganic salts easily absorbed through skin

Adverse effects: Facial burns, skin discolouring, neurotoxicity, renal toxicity

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10
Q

In the case studies for Pan Pharmceuticals what did the assay with the product Travacalm show?

A

10 fold variation in hyoscine, which can cause serious ADR like delirium

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11
Q

How did Slim10 enter the market?

A

They showed good batches for approval, then adulterated subsequent batches

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12
Q

What was Slim10 Adulterated with?

A
  1. Fenfluramine (trace amts)
  2. Thyroxine medications (must add thyroid lysing agent before it can be detected)
  3. Nitrosofenfluramine (Hepatotoxic analogue of fenfluramine)
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13
Q

What kind of Signs and sx manifested in patients who took Slim10?

A

Hyperthyroidism

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14
Q

What was the adulterant in some aphrodisiacs? (E.g. Power1 walnut, Counterfeit Cialis, etc.), and what was the AE that manifested in patients who took it?

A

Glibenclamide (about 40-100mg/tab, while therapeutic dose is 2.5-20mg OD)
AE: Neuroglycopenia

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15
Q

What was used as a marker of insulin for patients who presented with Neuroglycopenia after taking adulterated aphrodisiacs?

A

C-peptide

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16
Q

What are the common adulterants for:

  1. Virility products
  2. Anti-inflammatory products
  3. Slimming products
A
  1. Virility: Sildenafil, Vardenafil, Tadalafil and their analogues
  2. Anti-inflammatory: Dexamethasone, NSAIDs
  3. Slimming Products: Sibutramine and its analogues
17
Q

Name some analogues of sildenafil. Why do unscrupulous manufactuers add analogues instead of the actual compound?

A

Homosildenafil, Thiohomosildenafil

To avoid lab detection

18
Q

Some future challenges of PV

A
  1. Opportunities in Genomic Era
  2. Emergence of Complementary Medicines
  3. Registries for Biological Products and Gene Therapy
  4. Forging Closer ties with international COunterparts
  5. Maximising IT tools for Signal Detection & Communication