<HashMap><database>biostudies-literature</database><scores/><additional><submitter>Jordan SC</submitter><funding>NHLBI NIH HHS</funding><funding>National Institutes of Health</funding><funding>NIH HHS</funding><pagination>e14182</pagination><full_dataset_link>https://www.ebi.ac.uk/biostudies/studies/S-EPMC10922395</full_dataset_link><repository>biostudies-literature</repository><omics_type>Unknown</omics_type><volume>26(1)</volume><pubmed_abstract>&lt;h4>Background&lt;/h4>Tixagevimab-cilgavimab (Tix-Cil) was authorized for prophylaxis against COVID-19 in immunocompromised patients from December 2021 through January 2023. Real-world effectiveness for solid organ transplant (SOT) recipients has been unclear.&lt;h4>Methods&lt;/h4>We enrolled 911 SOT recipients into a longitudinal COVID-19 serology study, of whom 381 (42%) received ≥1 dose of Tix-Cil. We collected and analyzed data on incident SARS-CoV-2 infections and antibody kinetics for all patients from January 2022 to March 2023, including periods dominated by Omicron BA and BQ subvariants.&lt;h4>Results&lt;/h4>Over 253 ± 131 days of follow-up, there were 324 new-onset SARS-CoV-2 infections: 117 (31%) in Tix-Cil treated and 207 (39%) in Tix-Cil untreated patients (p = .012). In analyses adjusting for demographic, clinical, and COVID-19 exposure factors, any Tix-Cil treatment was associated with lower infection risk (OR 0.52, 95% CI 0.27-0.96, p = .039) throughout the surveillance period including when more resistant BQ.1 and BQ.1.1 subvariants had emerged (12/1/2022 onwards). Among treated patients, receiving a Tix-Cil dose was associated with substantial and sustained increase in anti-spike IgG antibody and angiotensin-converting enzyme 2 binding inhibition levels (Abbott Architect assay) that together also demonstrated association with lower infection risk (p = .042). During the full surveillance period, the frequency of infections requiring hospitalization was low overall (N = 26, 2.9% of the total cohort) and not significantly different between Tix-Cil recipients (N = 12, 3.2% of treated patients) and non-Tix-Cil recipients (N = 14, 2.6% of untreated patients) with unadjusted p = .31 for between-group difference.&lt;h4>Conclusion&lt;/h4>In a large cohort of SOT recipients, we found that Tix-Cil reduced infection risk even amidst emergent Omicron subvariants. Additionally, the extent of measurable humoral response to Tix-Cil may indicate relative effectiveness. Pre-exposure monoclonal antibody therapy may represent a strategy that will continue to offer clinical benefit for immunocompromised persons who are known to derive limited protection from vaccinations.</pubmed_abstract><journal>Transplant infectious disease : an official journal of the Transplantation Society</journal><pubmed_title>Assessing the post hoc effectiveness of tixagevimab-cilgavimab for prevention of SARS-CoV-2 infections in solid organ transplant recipients.</pubmed_title><pmcid>PMC10922395</pmcid><funding_grant_id>R01 HL151828</funding_grant_id><funding_grant_id>K23HL153888</funding_grant_id><funding_grant_id>R01 HL131532</funding_grant_id><funding_grant_id>K23 HL153888</funding_grant_id><pubmed_authors>Prostko JC</pubmed_authors><pubmed_authors>Ebinger JE</pubmed_authors><pubmed_authors>Mendez M</pubmed_authors><pubmed_authors>Kittleson M</pubmed_authors><pubmed_authors>Bravo M</pubmed_authors><pubmed_authors>Frias E</pubmed_authors><pubmed_authors>Wang M</pubmed_authors><pubmed_authors>Cheng S</pubmed_authors><pubmed_authors>Jordan SC</pubmed_authors><pubmed_authors>Joung SY</pubmed_authors><pubmed_authors>Masoom H</pubmed_authors><pubmed_authors>Sun N</pubmed_authors><pubmed_authors>Sobhani K</pubmed_authors><pubmed_authors>Chang C</pubmed_authors><pubmed_authors>Patel J</pubmed_authors><pubmed_authors>Tran TA</pubmed_authors></additional><is_claimable>false</is_claimable><name>Assessing the post hoc effectiveness of tixagevimab-cilgavimab for prevention of SARS-CoV-2 infections in solid organ transplant recipients.</name><description>&lt;h4>Background&lt;/h4>Tixagevimab-cilgavimab (Tix-Cil) was authorized for prophylaxis against COVID-19 in immunocompromised patients from December 2021 through January 2023. Real-world effectiveness for solid organ transplant (SOT) recipients has been unclear.&lt;h4>Methods&lt;/h4>We enrolled 911 SOT recipients into a longitudinal COVID-19 serology study, of whom 381 (42%) received ≥1 dose of Tix-Cil. We collected and analyzed data on incident SARS-CoV-2 infections and antibody kinetics for all patients from January 2022 to March 2023, including periods dominated by Omicron BA and BQ subvariants.&lt;h4>Results&lt;/h4>Over 253 ± 131 days of follow-up, there were 324 new-onset SARS-CoV-2 infections: 117 (31%) in Tix-Cil treated and 207 (39%) in Tix-Cil untreated patients (p = .012). In analyses adjusting for demographic, clinical, and COVID-19 exposure factors, any Tix-Cil treatment was associated with lower infection risk (OR 0.52, 95% CI 0.27-0.96, p = .039) throughout the surveillance period including when more resistant BQ.1 and BQ.1.1 subvariants had emerged (12/1/2022 onwards). Among treated patients, receiving a Tix-Cil dose was associated with substantial and sustained increase in anti-spike IgG antibody and angiotensin-converting enzyme 2 binding inhibition levels (Abbott Architect assay) that together also demonstrated association with lower infection risk (p = .042). During the full surveillance period, the frequency of infections requiring hospitalization was low overall (N = 26, 2.9% of the total cohort) and not significantly different between Tix-Cil recipients (N = 12, 3.2% of treated patients) and non-Tix-Cil recipients (N = 14, 2.6% of untreated patients) with unadjusted p = .31 for between-group difference.&lt;h4>Conclusion&lt;/h4>In a large cohort of SOT recipients, we found that Tix-Cil reduced infection risk even amidst emergent Omicron subvariants. Additionally, the extent of measurable humoral response to Tix-Cil may indicate relative effectiveness. Pre-exposure monoclonal antibody therapy may represent a strategy that will continue to offer clinical benefit for immunocompromised persons who are known to derive limited protection from vaccinations.</description><dates><release>2024-01-01T00:00:00Z</release><publication>2024 Feb</publication><modification>2025-04-03T23:21:21.368Z</modification><creation>2025-04-03T23:21:21.368Z</creation></dates><accession>S-EPMC10922395</accession><cross_references><pubmed>37885435</pubmed><doi>10.1111/tid.14182</doi></cross_references></HashMap>