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LINEAGE DETERMINATION ISSUE #1770
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Hi @noutin2020, I had the same issue and @AngieHinrichs helped me with this: Hope this helps!! |
Hi @noutin2020, it can happen that Usher and Nextclade show somewhat different results. In this case, the difference between XBB.1 and XBB.1.5 is small and depends on just a single to a few nucleotide substitutions. When the sequence is incomplete (having some Ns), it is possible that the exact lineage cannot be determined with certainty. Likewise, sometimes there are bioinformatic analysis artefacts that can make it difficult for the algorithms to be certain about which exact lineage it is. If you share the sequence I could have a look and see why the two tools disagree (slightly). Based on the sampling date and location you provided, it is quite likely that the sample is XBB.1.5 (or another XBB with S:F486P), see covSpectrum graphic showing proportion of XBB* that is XBB.1.5 in Africa in the past 3 months:
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Hello @corneliusroemer, In addition, it has S:F486P mutation. Since you mentioned that it could be another XBB with S:F486P, which one could it be? I look forward to hearing from you. |
Hi the one on left is XBB.1.5 , the other on the right is part of a fast undesignated lineage that emerged in africa proposed in #1712 |
It's an XBB.1 with S:F486P - but without the T17124C usually found in XBB.1.5 (though not in 100%). So it could be XBB.1.5, but could also be an independent acquisition of S:F486P. Nextclade calls it XBB.1.5 because it does fit the broad definition: XBB.1 + S:F486P. Though this could be a false positive. Usher finds this in a cluster of XBB.1 with S:F486P that is not labelled XBB.1.5. I'll have to study this part of the tree more closely to see whether this should be XBB.1.5 or is a genuinely independent XBB.1 + S:F486P. There could already be an issue for this. |
@corneliusroemer it is part of #1712 (i strongly support designation of it, second fastest in the world after XBB.1.16) |
Very insightful discussion and thank you so much for your time. @corneliusroemer , it is not a false positive because fresh sample with very good ct value. Independent acquisition of S:F486P?? I am curious, shed more light on this statement, please. @FedeGueli, about your strong recommendation: Is it a general recommendation or specific to this sequence? How can this designation be done? |
It was a message for Cormelius, only the pango team could do designations, and designations are always about a lineage not a singlet sequence as stated in #1 . By the way now it has been designated XBB.1.17.1 so your sequence on the right belongs to this lineage. |
Thank you for concluding nicely this discussion.
Let's keep in touch!
…On Sun, Mar 19, 2023, 14:41 Federico Gueli ***@***.***> wrote:
@FedeGueli <https://github.com/FedeGueli>, about your strong
recommendation
Is it a general recommendation or specific to this sequence?
How can this designation be done?
It was a message for Cormelius, only the pango team could do designations,
and designations are always about a lineage not a singlet sequence as
stated in #1 <#1>
.
By the way now it has been designated XBB.1.17.1 so your sequence on the
right belongs to this lineage.
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@noutin2020 |
Ok. Rather sequencing run (not PCR). Thanks |
After analysing the Whole Genome Sequence of a positive SARS-CoV-2 sample collected on 31/01/2023,
I determined the lineage of the strain using both Nexclade and Pangolin
The Output of Nexclade was: XBB.1.
The Output of Pangolin was: XBB.1.5(1/1) with the following note:
scorpio lineage BA.2 conflicts with inference lineage XBB.1.5,4.2,v1.18.1.1
How can I interpret this note and make final decision on the lineage of this variant?
Your various responses will be highly appreciated!
I look forward to hearing from you.
Regards,
Noutin
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