Overview of the Diagnostic Approach in the Pediatric Genetics Clinical Setting Flashcards
You are caring for a 5 yr old boy with multiple congenital anomalies with suspected
genetic contribution.
You ordered chromosome microarray analysis, which revealed a 3.4 Mb deletion of
the 17pter and 5.6 Mb duplication of the 17qter. Which of the following parental
chromosomal abnormalities is most likely to lead to this finding?
A. balanced reciprocal translocation
B. balanced Robertsonian translocation
C. isochromosome
D. pericentric inversion
E. paracentric inversion
D - pericentric inversion
not balanced reciprocal trnaslocation because it would be 2 different chromosomes
not balanced Robertsonian translocation because it’s not acrocentric chromosomes
not isochromosome becaue entire arm of p or q would be missing
not paracentric becuase on two different arms of the chromsome I think.
You are evaluating a child with lissencephaly (brain anomaly), microcephaly, dysmorphic features, cardiac malformations, hypoplastic male external genitalia, growth retardation, and intellectual disability with seizures and EEG abnormalities.
You ordered chromosome microarray analysis (CMA), and the results showed a 2.5
Mb duplication of 10pter and a 3.4 Mb deletion of 17pter. What parental chromosome abnormality is likely to result in such CMA result in the child?
A. Balanced insertion
B. Balanced paracentric inversion
C. Balanced pericentric inversion
D. Balanced reciprocal translocation
E. Robertsonian translocationrsion
D. Balanced reciprocal translocation because it is a deletion and duplication of 2 different chromsomes
When there is a balanced translocation (between 2 chromosomes) in order for pairing up in meiosis to occur, a quadrivalent alignment happens. The gametes that result from this ‘pairing’ of 4 chromosomes is….
Adjacent-1 and Adjacent-2 segregation result in unbalanced gametes. Alternate segregation results in normal or balanced gametes.
In alternate segregation:
non-homologous
centromeres travel to
opposite poles (leads to
gametes with a complete
genetic complement)
In adjacent-1, homologous
centromeres travel to
separate daughter cells
In adjacent-2(uncommon)
adjacent chromosomes with
homologous centromeres go
to the same daughter cell
Explain the following findings in a child :
* arr1q44(245956212-249212668)x1
* arr18q22.2q22.3(67832679-71931611)x1
Mother is asking about recurrence risk, of note she now has a different partner.
What would be the next step ?
- test the parents
- these are small deletions so CMA would be best test
- FISH would be option too since we know what we are looking for
FISH testing done after CMA result of child.
Maternal:
* ish1q44(RP11-230L4x2)
* ish18q22.3(RP11-630H13x1)
Paternal:
* ish1q44(RP11-230L4x2)
* ish18q22.3(RP11-630H13x2)
Explain what method was used, what are the findings and what is the recurrence
risk for future pregnancies
- FISH probes made from child’s DNA
- Mom has 1 deletion that is in the child, so recurrence risk = 50%
- The other deletion is de novo, so recurrence risk = 1-2%
What testing should be ordered for multiple congenital anomalies?
WES/CMA or WGS as 1st or 2nd tier
it is recommended to go broad
In the NICU setting is often best to go with what testing?
rapid genome
if specific you can go with panel however if kid is deteriorating this could be wasting time if you are not sure
When to order karyotype?
Mainly used for aneuploidies, to look for translocations (e.g.
Robertsonian translocation for down syndrome), or other rearrangements (ring
chromosome, isochromosome)
When to order CMA?
can be used as first tier for multiple congenital anomalies/DD/ID/learning
disability/Autism Spectrum/dysmorphic features/behavioral concerns, or when there is concern for specific CNV diagnosis (22q11.2 etc)
- issue with CMA is that it’s a start. if only CMA done and nothign found other can think genetic testing was done adn no further testing is needed.
I don’t think Dr. Tallis would recommend that we order CMA alone? I’m not sure.
Multiple congenital anomalies/DD/ID/learning disability/Autism Spectrum
Disorders- per ACMG practice guidelines
What test to order?
go broad with CMA/WES or WGS
Is mitochondrial DNA sequencing included in WGS?
Mitochondrial DNA sequencing is included in WGS
When is the only time it is appropriate to order single gene testing?
known familial mutation
When is the use of panels appropriate?
Use of panels can be more prevalent when evaluating adults versus infants/children, as the phenotype is often clearer
panels shoudl include sequencing and del/dup anlysis
VUS rate is actually higher with panels in comparison with WGS/WES. Why is this?
The lab reports everything they find in a panel. WGS/WES would find too many to report them all. Only report what is relevant to reporting criteria.
Unexpected findings including secondary findings are more common with broader
testing (WES/WGS)
Just improtant to remember.
