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Includes a long Covid subgroup with ME/CFS
pmc.ncbi.nlm.nih.gov
Open Forum Infect Dis
. 2026 Jan 11;13(Suppl 1)
faf695.1837. doi: 10.1093/ofid/ofaf695.1837
PMCID: PMC12793287
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Clinical lab abnormality level, as defined by percent of patients with abnormal lab result at anytime (initial visit or follow-up), compared between the long covid positive for MECFS (MECFS), post-vaccination syndrome (PVS), and long covid negative for MECFS (LC) groups and previously reported positivity rates in healthy populations. Histamine: plasma histamine level, Tryptase: plasma tryptase level, IL 2 receptor: interleukin 2 receptor (CD25), IL 10: interleukin 10, IL 13: interleukin 13, TNF-alpha: tumor necrosis factor alpha, CD4+ T Cells: quantitative CD3+/CD4 lymphocytes, CD8+ T Cells: quantitative CD8+ lymphocytes, HSP70: heat shock protein-70 IgG western blot, ACL: quantitative anticardiolipin IgM, Anti U1-RNP: quantitative ribonucleic protein extranuclear antibody IgG. Reference ranges: Histamine: 0-8 mmol/L, Tryptase: <=10.9 ug/L, IL 2 receptor 175.3-858.2 pg/mL, IL 10: <=2.8 pg/mL, IL 13 <=2.3 pg/mL. TNF-alpha <=7.2 pg/mL, CD4+ T Cells: 393-1489 cells/uL, CD8+ T Cells: 148-788 cells/uL, HSP70: Negative, ACL: <=12 MPL, Anti U1-RNP: <1.0 U
P-1662. Post-Acute Sequelae of COVID-19 and Post-COVID-19 Vaccination Syndrome: A Comparison of Clinical Immune Biomarkers - PMC
Post-acute sequelae of COVID-19 (PASC), and post-COVID-19 vaccination syndrome (PVS) present overlapping but distinct clinical challenges. Immunologic biomarker abnormalities have previously been established in PASC but less so in PVS. This study ...
pmc.ncbi.nlm.nih.gov
Open Forum Infect Dis
. 2026 Jan 11;13(Suppl 1)
faf695.1837. doi: 10.1093/ofid/ofaf695.1837P-1662. Post-Acute Sequelae of COVID-19 and Post-COVID-19 Vaccination Syndrome: A Comparison of Clinical Immune Biomarkers
Thomas Heisler 1, Lawrence Purpura III 2, Michael Yin 3, Steven Palmer 4, Jayesh Shah 5, Ga Young Seo 6, Abigail Graham 7, Antonia Sturiza Saint Jean 8, Xiomara Javier 9, Giselle S Pinto 10, Joan Bosco 11, Karl Reis 12, Magdalena E Sobieszczyk 13, Amanda R Castillo 14,1,2- Author information
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PMCID: PMC12793287
Background
Post-acute sequelae of COVID-19 (PASC), and post-COVID-19 vaccination syndrome (PVS) present overlapping but distinct clinical challenges. Immunologic biomarker abnormalities have previously been established in PASC but less so in PVS. This study aims to distinguish immunologic biomarker patterns in PASC and PVS.Figure 1.
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Clinical lab abnormality level, as defined by percent of patients with abnormal lab result at anytime (initial visit or follow-up), compared between the long covid positive for MECFS (MECFS), post-vaccination syndrome (PVS), and long covid negative for MECFS (LC) groups and previously reported positivity rates in healthy populations. Histamine: plasma histamine level, Tryptase: plasma tryptase level, IL 2 receptor: interleukin 2 receptor (CD25), IL 10: interleukin 10, IL 13: interleukin 13, TNF-alpha: tumor necrosis factor alpha, CD4+ T Cells: quantitative CD3+/CD4 lymphocytes, CD8+ T Cells: quantitative CD8+ lymphocytes, HSP70: heat shock protein-70 IgG western blot, ACL: quantitative anticardiolipin IgM, Anti U1-RNP: quantitative ribonucleic protein extranuclear antibody IgG. Reference ranges: Histamine: 0-8 mmol/L, Tryptase: <=10.9 ug/L, IL 2 receptor 175.3-858.2 pg/mL, IL 10: <=2.8 pg/mL, IL 13 <=2.3 pg/mL. TNF-alpha <=7.2 pg/mL, CD4+ T Cells: 393-1489 cells/uL, CD8+ T Cells: 148-788 cells/uL, HSP70: Negative, ACL: <=12 MPL, Anti U1-RNP: <1.0 U