Difference between revisions of "Libre Pathology talk:Study Group"

From Libre Pathology
Jump to navigation Jump to search
 
(6 intermediate revisions by the same user not shown)
Line 48: Line 48:
[[User:Michael|Michael]] ([[User talk:Michael|talk]]) 23:43, 25 October 2014 (EDT)
[[User:Michael|Michael]] ([[User talk:Michael|talk]]) 23:43, 25 October 2014 (EDT)


== Short answer questions on genetics and molecular pathology.  ==
= [[Short answer questions submitted by Tate]]=
 
These are some questions I came up with that are plausible to me... let me know if they are out to lunch.
 
==[[Molecular Pathology Rotation Notes]]==
 
==[[Robbins and Cotran 9th Edition Questions]]==
 
{{hidden|MC cause of spontaneous abortion is ?|<center>[[ A demonstrable chromosomal abnormality.]]</center>}}
 
{{hidden|1% of all newborn infants possess a gross chromosomal abnormality and 5% of people <25y present with  |<center>[[a genetic disease. ]]</center>}}
 
{{hidden|Mutation|<center>[[permanent change in the DNA, if affect germ cells are transmitted to the progeny ]]</center>}}
 
{{hidden|List and describe 4 broad categories of human genetic disorders:|<center>[[Disorders related to mutation sin single genes with large effects i. Usually follow classic Mendelian pattern of inheritance
ii. Often highly penetrant (large proportion of pop with gene has disease)
b. Chromosomal disorders
i. Structural or numerical alterations in autosomes and sex chromosomes
ii. Uncommon, high penetrance
c. Complex multigenic disorders
i. Interactions between multiple variant forms of genes and environmental factors (polymorphisms), poly genic means disease when many polymorphism present
d. Single gene disorders with nonclassic patterns of inheritance (not mendelian)
i. Disorders resulting from triplet repeat mutations
ii. Mutations in mitochondrial DNA
iii. Those influenced by genomic imprinting
iv. Those influenced by gonadal mosaicism]]</center>}}
 
{{hidden|List and describe the possible outcomes of a point mutation in a coding region?|[[a. Missense mutation – pt mutation changes amino acid code, conservative when the amino acid is preserved, non conservative when replaced with another amino acid, b. Nonsense mutation – makes a stop codon ]]</center>}}
 
{{hidden|List and describe the possible outcomes of point mutation or deletion in a non-coding region.|<center>[[a. Promoters/enhancers – interfere with binding of transcription factors, marker reduction or total lack of transcription, b. Introns – defective splicing > failure to make mature RNA > no translation]]</center>}}
 
{{hidden|List and describe the possible outcomes of deletions and insertions.|<center>[[a.Small coding: not multiple of three = frameshift, if multiple of 3 than add or del amino acids accordingly, often premature stop codon
i. Tay Sachs disease: 4 base pair insertion in Hexosaminidase A gene ]]}}
 
{{hidden|List and describe the possible outcomes of trinucleotide repeat mutations.|[[a. Usually G&C, dynamic and increase during gametogenesis, “RNA stutters”,b. Fragile X – CGG 250-4000, Huntinton’s Disease ]]}}
 
{{hidden|List and describe three examples of inheritance of single gene mutations|[[a. AD – manifested in the heterologous state, one parent of index case is usually affected, males and females affected and both can transmit conditioni. De novo cases may not have affected parentii. Penetrance = fraction of people with gene who have the traitiii. Variable expressivity = those with mutant gene have variety of phenotypesiv. Often age of onset is delayed so can reproduce before die from diseasev. Biochem mechanisms1. Reduced production of a protein or dysfunctional/inactive protein2. Involved in regulation of complex metabolic pathyway subject to feedback inhibition3. Key structural proteins (collagen and cytoskeleton of RBC)a. May be a dominant negative , e.g. osteogenesis imperfecta4. Gain of function are rare, 2 formsa. Increased in proteins normal function (excess enzyme activity)b. Huntinton’s diseas (abn protein accumulates, toxic to neurons)b. ARi. Largest category – both alleles at a locus are mutated1. Expression is uniform, complete penetrance common, early onset, unaffected carrier family members, mostly enzymesc. X Linkedi. All sex linked, and almost all are recessive , if Y Chromosome affected usually infertile males > no progenyii. Male expression b/c hemizygous, daughter carriers with variable phenotype because of lionization of 2nd X e.g G6DPiii. Dominant . vitamin D resistant rickets]]</center>}}
 
Stopped at P142
 
=== Molecular Genetic Diagnosis===
{{hidden|List three basic molecular diagnostic techniques|[[a. Karyotyping, b. Southern blot, c. Sanger DNA sequencing, d. Polymerase chain reaction]]}}
 
 
===CAP Molecular Diagnosis of Lung Cancer===
 
{{hidden|List 5 treatment defining molecular transformation, the neoplasm, and the genetic alteration|[[1. 100% of CML: BRR-ABL > Imatinib, 2. 20% of Lung Adenocarcinoma: EGFR > Erlotinib/Gefitinib, 3. 25% Infiltrative ductal carcinoma of breast HER2>Trastuzumab, 4. 50% of Melanoma, BRAF v600E > PLX4032, 5. 4% of Lung Adenocarcinoma: ALK > Crizotinib]]}}
 
{{hidden|List and describe 5 areas of Genetic characaterization of tumours for personalized medicine|[[DNA mutations, DNA chromosomal alterations, mRNA and MiRNA profiling, Proteomics, DNA epigenetics]]}}
 
{{hidden|What fraction of Lung adenocarcinomas have no known detactable mutations|[[42%]]}}
 
{{hidden|What are the three most common molecular alterations of Lung Adenocarcinoma|[[KRAS 23%, EGFR 15%, TP53 5%]]}}
 
{{hidden|What is the two most common molecular alteration makes patients with EGFR mutations resistant to targetted therapies?|[[KRAS (primary) and T790M (primary and acquired)]]}}
 
{{hidden|List two EGFR kinase inhibitors.|[[Gefitinib/Iressa, Erlotinib/Tarceva]]}}
 
{{hidden|What are the three most common cancers associated with KRAS mutations?|[[Pancreatic 90%, Colon 50%, Lung NSCLC 30%]]}}
 
{{hidden|Why don't KRAS + tumours respond to Anti EGFR therapies?|[[KRAS is downstream from EGFR, so changing the function of EFGR would not have any effect on mutated KRAS]]}}
 
{{hidden|Explain the cost effectiveness of genetic testing for targetted therapies?|[[Most molecular tests cost $200-1000, vs one month of targetted therapy $2000-10000/month]]}}
 
{{hidden|What are the three most common cancers associated with BRAF mutations?|[[Melanoma 70%, Papillary Thyroid Carcinoma 50%, Ovarian serious carcinoma 30%, Colon cancer 10%, Hint Papillary architecture]]}}
 
{{hidden|Beta catenin/CTNNB1 expression is found with which histological pattern of lung adenocarcinoma?|[[Low grade adenocarcinoma of fetal type, poor px, <40yo, and has glycogen rich glandular formations, may occur in FAP patients]]}}
 
{{hidden|What is the most common ALK rearrangement found in NSCLC?|[[EML4-ALK (90% of the 13% of lung cancers found to due to ALK fusions)]]}}
 
{{hidden|List some pros and cons of ALK FISH.|[[Pros: commercial FDA approved probes available, not too expensive, moderately easy to disseminate screening, clinically validated, and failed tests on poorly preserved tissues are not reported as negative. Cons: need fish lab expertise (including pathologist and PhD), can be tricky if genes are close]]}}
 
{{hidden|List some pros and cons of ALK IHC.|[[Pros: fast, cheap, easy to disseminate screening, Cons: commercial antibodies sub-optimal, poorly preserved tissues (esp bx) may give false negative results due to loss of antigenicity, no internal control]]}}
 
{{hidden|What is a positive count in the ALK-FISH?|[[Signal split >2 probe diameters]]}}
 
===CAP Molecular Diagnosis of AML===
 
{{hidden|List 6 genes associated with Acute Myeloid Leukemia that have been identified by cloning translocation break points|[[RUNX1, RUNX1T1, PML, CBFB, ETV6, MLL]]}}
 
{{hidden|List the 5 main categories of classification of Acute Myeloid Leukemia|[[1. AML with recurrent genetic abnormalities, 2. AML with myelodysplasia-related changes, 3. Therapy related myeloid neoplasms, 4. AML, NOS, 5. Myeloid sarcoma]]}}
 
{{hidden|Give any three translocations identified in AML.|[[t(8,21), inv (16), t(15,17), t(9,11), t(6,9), inv(3), t(1,22), mutated NPM1, mutated CEBPA]]}}
 
{{hidden|What entities are fall under the AML, NOS classification?|[[AML with minimal differentiation, AML without maturation, AML with maturation, Acute myelomonocytic leukemia, Acute monoblastic/monocytic leukemia, Acute erythroid leukemias (pure erythroid, erythroleukemia, erythroid/myeloid), Acute Megakaryoblastic leukemia, Acute basophilic leukemia, Acte panmyelosis with myelofibrosis]]}}
 
{{hidden|List 2 genes which confer a poor prognostic impact vs 2 which confer a good prognostic impact.|[[Poor: KIT, FLT3, Good: NPM1, CEBPA]]}}
 
 
=== CAP Breast Cancer and Molecular ===
 
{{Hidden|List 3 patient and 4 tumour features that affect Prognosis and treatment.|[[Patient: age, menstual status, comorbidities; Tumour factors: N status, LVI, size, grade]]}}
 
{{hidden|Describe the histological grading system used for breast cancer.|[[Nuclear pleomorphism, mitoses, and mitotic index (each scored 1-3), with cumulative grade 1(score 3-5), grade 2(score 6-7), and grade 3 (score 8-9)]]}}
 
{{hidden|Describe the genomic grading system used for breast cancer.|[[Low grade path (+1q, -16q), High grade (17q12, 11q13, nad 1p21-p25)]]}}
 
{{hidden|What defines a positive ER by IHC for the purpose of determining Tamoxifen therapy?|[[>=1% of invasive tumour cells nuclear positivity]]}}
 
{{hidden|what defines a positive HER2 for the purpose of treatment with Herceptin?|[[HER2 IHC >30% with complete membranous staining OR HER2/CEP17 >2.2]]}}
 
{{hidden|What are the indications for chemotherapy for breast cancer patients?|[[Low expression of ER/PR, Grade 3 histology, Ki67>20%, 4+ nodes positive, +LVI, and tumour >5cm]}}
 
{{hidden|What are the indications for hormonal therapy alone?|[[high expression of ER, Grade 1, Ki67>40%, Node negative, LVI not identified, and tumour 1-2cm]]}
 
{{hidden|What are the four categories of breast cancer using the molecular classification of gene expression?|[[Luminal A, Luminal B, Basal, and Her2 OverExpression]]}}
 
{{hidden|What is the difference between unsupervised and supervised molecular classification of tumours?|[[Supervised is based on seperating patients by clinical features (e.g. progression) and trying to identify common molecular characteristics within those groups. Unsupervised is the opposite, tumours are grouped by common molecular features and their behaviour examined based on these groups.]]}}
 
{{hidden|What are the four groups and list one gene for each used in the Oncotype Dx 21 Gene prognostic model.|[[Invasion (Cathespin L2, Stromolysin), HER2 (Her2, GRB7), ER (BCL2, SCUBE2, ER, PR), Proliferation (Cyclin D1, Ki67, MYBL2, STK15, Survivin)]]}}
 
{{hidden|What are the features of Luminal A breast cancer?|High ER/PR expression, low histological grade, low levels of proliferative genes, HER2neg, indolent clinical course, better prognosis, Tamoxifen responders, low recurrence score Oncotype Dx, minimal benefits of adjuvant chemotherapy.]]}}
 
{{hidden|What are the features of Luminal B breast cancer?|low ER/PR expression (may be PR neg), over expression GFR(Her2 & EGFR), higher histological grade, more aggressive clinical course, worse prognosis, more likely positive lymph nodes, and high expression of proliferative genes (Ki67)]]}}
 
{{hidden|What are the features of Luminal B HER2|[[ ER+, HER2+, agressive clinical course, decrease response to tamoxifen, may benefit from chemo and tamoxifen, increased recurrence risk Oncotype Dx Score, some may benefit form Herceptin+Chemo+Tamoxifen]]}}
 
{{hidden|What are the features of Her2 Enriched breast cancers?|[[ GEP are ER neg, over expression of other genes in HER2 aplification, high proliferative index, increased probability of P53 mutation, high histological grade, younger age, agressive clinical course, Poor Px, good response to herceptin in combination with chemo, pathological complete response to chemo+herceptin]]}}
 
 
{{hidden|What are the features of Basal breast cancer?|[[]]}}

Latest revision as of 13:29, 12 August 2015

Michael's thoughts on the exam

  • I wrote it and passed it in 2012. I also did the American exam the same year and passed that.
  • The pass rate for the FRCPC exam is pretty high.
    • 2009-2011 it was 96+/-3.9% for Canadian medical school grads on their first attempt.

Written

  • I though it was picking at details. Some things are very relevant to practise... other less so.
    • The pocketbook version of Robbins covers most of it.

Practical (slide) exam

  • You should know the answer almost immediately.
    • If you don't know, write something down and move on.
  • It is set to broadly cover everything.
  • If it isn't a spot diagnosis... it should not be on.
  • Somethings are PGY2/PGY3 stuff. One should not overthink things.
  • Anecdotally, the first impression is usually the right one.
    • I think one should stick with the first impression.

Gross exam

  • Go with the most probable if you're uncertain.
  • I worked through the Atlas of Gross Pathology with Histologic Correlation (see Pathology books for the reference).
    • I am not sure this is necessary... but I thought it was useful.
  • Flickr.com/Google images has a lot to offer in this respect.
  • Gross spot diagnosis.

Forensic exam

  • I thought this was tricky... and I liked forensics.
  • Residents that took the exam prior to me said the same.

Cytology exam

  • Some of the cases have several images.
  • I remember being confused... the first three images were from one case. I remember thinking... I have the same diagnosis three times.
  • Like the forensics and gross sections - this section isn't too long. From an exam strategy point-of-view, this makes it less likely that a diagnosis is repeated.

Oral exam

  • I think this is to test if you are safe and useful.
    • By "safe" I mean: knowing your limits and consulting with a colleague when appropriate.
    • By "useful" I mean: you don't need to consult on everything.
  • The examiners ask a pre-determined list of questions.
    • Questions may depend on one another and, in fairness, they are told to redirect you.
      • Example: You see a lung biopsy with hyaline material... and you go down the fibrosis route-- but it is really amyloidosis.
        • The examiners will say something like "how would one work-up suspected amyloid?" or "lets assume this is amyloid..."
  • If you're a Canadian resident, you cannot be examined by someone within your residency program.
  • As far as I know, examiners are told to be stone-faced, i.e. show no emotion.
  • Some of the cases were very straight forward.
  • I didn't think anything was really exotic.

Michael (talk) 23:43, 25 October 2014 (EDT)

Short answer questions submitted by Tate