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Monkeypox Virus Controls
SARS-CoV-2 Controls
cfDNA Pan-cancer

Monkeypox Virus Controls

What are the Twist Synthetic Monkeypox Virus Controls?
What are the concentrations of the Monkeypox controls?
How are the monkeypox controls qualified?
What are the full sequences/breakpoints of the Monkeypox controls?
What is the storage temperature for the monkeypox controls?
What fraction of the genome is covered by the monkeypox controls?
Which variants are covered and how many fragments (and sizes) are in each control?
What protocol do you recommend using with the monkeypox controls?
What starting input would you recommend for the monkeypox controls?
Why can’t I directly order the monkeypox control on your website?
Does Twist make synthetic controls for other viruses?
Are these controls ISO certified?
Why is only 80-85% of the genome covered instead of 100%?

SARS-CoV-2 Controls

What is the shelf life of Twist's RNA Controls?
Are the RNA Controls and Panel clinically approved?
What buffer is used in the SARS-CoV-2 RNA controls?

cfDNA Pan-cancer

What is your background cfDNA made from?
Is your background cfDNA limited supply?
Is background cfDNA from a mixed pool of donors?
Are these control oligos, RNA, what is in it/ components?
Does your product have matrics (e.g., synthetic plasma, plasma)?
Do you shear donor derived background?
Is there any concern for introduced bias for the expansion of cfDNA?
How do you design the ctDNA/ variant list?
What is the structure of the 3' and 5'?
What is the WGS and WES setting to qualify the cfDNA material, and QC the Twist cfDNA?
Were the mutations in the standards confirmed by NGS as well, as with digital PCR as it says in the document?
How do we know we are very close to natural background cfDNA?
What is the recommend input and dilution buffer?
Can’t find indel or other hard to detect variants?
What reagents (e.g., library prep) do you use for the liquid biopsy workflow?
Do you recommend to pool this control with patient sample after library prep, before NGS?
Are there different needs between amplicon and hybrid capture customers?
Variant (COSM214499) is always high in 0% in NGS QC results, why?
For NGS QC, do you use target capture sequence for the 458 variants or use a whole genome sequence?

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