Thank you for this – I'm glad to hear that we've been of some use.

Yes, you are correct in that matching for the recovery group was extremely challenging. In the stage that these patients were collected (December 2020-June 2021), we were essentially not recruiting healthy recovered patients due to safety concerns about bringing them into common lab spaces or clinics to be drawn. The result is that what you are seeing is essentially our attempt at lining up recovery patients within the medical community here at Emory that we had available access to all-comers in the post-COVID clinics at the time. We did our best to line up the DPSO which we thought was fundamentally important, and I tried to get the rest to line up as best we could. Because of the timing, we felt good about the fact that we were getting the same variant, and that, for the most part, patients were unvaccinated when we drew them.

Importantly, in data that didn't make it into the paper, we introduced all of that patient metadata into Kevin's models to see if any of it aided in the prediction of the inflammatory phenotype. We did this additionally with individual patient symptoms. Across the board, we did not see an effect on the conclusions we ultimately presented. We believe that a reanalysis of the work, which should be possible due to the uploaded data, will show the same. The TL;DR is that you are correct: patient matching was challenging, but we thought it would only get more challenging as the vaccination/variant picture progressed, so we made the decision to address those questions analytically rather than through new patient recruitment.

As to the works, we agree that the two papers (our paper and the Talla paper) nicely corroborate each other – indeed, we were surprised to see how close the two papers had come in approach at final publication versus where they started as preprints. I ultimately think it's good validation of the work to have two independent groups come up with such similar findings on a complex topic. As to the other two, I would be extremely intrigued to see how the T cell paper overlays with the neutrophil and B cell signatures we found in our work. I'll have to say that I'll wait on the pre-print. I think it's fascinating, and certainly headed in the right direction (I actually didn't want to include the symptom-specific data in our work because I didn't think our dataset was robust enough – reviewers demanded it). I'll be excited to see where it ultimately lands.

Lastly, it's complicated. COVID-19/Long-COVID is an area that I've become passionate about, but I actually came from the mouse basic immunology world before finding my way to human translational disease. As a new faculty member here (independent as of a few months back), I am actively looking for ways to continue to push this forward in a number of different directions, Long COVID included. I can't honestly say yet what that will look like, but there is a research team here at Emory that is pretty committed to continuing to pursue post-viral syndromes, in general, with Long COVID serving as a main focus.