TY - JOUR
T1 - Sepsis subtypes and differential treatment response to vitamin C: Biological sub study of the LOVIT Trial
AU - LOVIT Investigators, the Canadian Critical Care Trials Group
AU - Rynne, J.
AU - Mosavie, M.
AU - Masse, Marie-Helene
AU - Menard, Julie
AU - Battista, Marie-Claude
AU - Maslove, David M
AU - del Sorbo, Lorenzo
AU - St-Arnaud, Charles
AU - DAragon, Frederick
AU - Fox-Robichaud, Alison
AU - Charbonney, Emmanuel
AU - Adhikari, Neill K.J.
AU - Lamontagne, François
AU - Shankar-Hari, M.
PY - 2025/1/7
Y1 - 2025/1/7
N2 - Purpose: We hypothesised that the biological heterogeneity of sepsis may highlight sepsis subtypes with differences in response to intravenous vitamin C treatment in the Lessening Organ Dysfunction with VITamin C (LOVIT) trial. Our aims were to identify sepsis subtypes and to test whether sepsis subtypes have differences in treatment effect to vitamin C and describe putative biological effects of vitamin C treatment. Methods: We measured biomarkers of inflammation, at baseline and at 7 days post-randomisation, in 457/863 (53.0%) of participants with plasma samples in the LOVIT trial. We used agglomerative hierarchical clustering on log
10-transformed baseline data of 26 biomarkers to identify sepsis subtypes. We analysed differences in vitamin C treatment effect with regression models incorporating robust standard errors to report odds ratio and 95% confidence intervals (OR(95% CI)). All analyses were completed blinded to treatment allocation. Results: Our cohort included 233/429 (54.3%) allocated to vitamin C and 224/434 (51.6%) allocated to placebo. A three-subtype model best explained the variance in our data. Subtype-2 had the highest, and subtype-3 had the lowest levels of inflammatory response. In paired longitudinal samples, vitamin C did not have discernible anti-inflammatory effects, with anti-inflammatory effects related to time since randomisation and concomitant hydrocortisone treatment. The treatment effect estimates (OR (95% CI)) for subtype-1, subtype-2 and subtype-3 were 1.04 (0.63–1.73), 1.33 (0.53–3.36) and 1.95 (0.85–4.49), respectively (test of heterogeneity p = 0.002). Conclusion: We report three sepsis subtypes based on inflammatory response profile. No subtype benefitted from vitamin C treatment in the LOVIT trial, with heterogeneity of treatment effect in the magnitude of harm. Trial registration: Funded by the Lotte and John Hecht Memorial Foundation; LOVIT ClinicalTrials.gov number, NCT03680274.
AB - Purpose: We hypothesised that the biological heterogeneity of sepsis may highlight sepsis subtypes with differences in response to intravenous vitamin C treatment in the Lessening Organ Dysfunction with VITamin C (LOVIT) trial. Our aims were to identify sepsis subtypes and to test whether sepsis subtypes have differences in treatment effect to vitamin C and describe putative biological effects of vitamin C treatment. Methods: We measured biomarkers of inflammation, at baseline and at 7 days post-randomisation, in 457/863 (53.0%) of participants with plasma samples in the LOVIT trial. We used agglomerative hierarchical clustering on log
10-transformed baseline data of 26 biomarkers to identify sepsis subtypes. We analysed differences in vitamin C treatment effect with regression models incorporating robust standard errors to report odds ratio and 95% confidence intervals (OR(95% CI)). All analyses were completed blinded to treatment allocation. Results: Our cohort included 233/429 (54.3%) allocated to vitamin C and 224/434 (51.6%) allocated to placebo. A three-subtype model best explained the variance in our data. Subtype-2 had the highest, and subtype-3 had the lowest levels of inflammatory response. In paired longitudinal samples, vitamin C did not have discernible anti-inflammatory effects, with anti-inflammatory effects related to time since randomisation and concomitant hydrocortisone treatment. The treatment effect estimates (OR (95% CI)) for subtype-1, subtype-2 and subtype-3 were 1.04 (0.63–1.73), 1.33 (0.53–3.36) and 1.95 (0.85–4.49), respectively (test of heterogeneity p = 0.002). Conclusion: We report three sepsis subtypes based on inflammatory response profile. No subtype benefitted from vitamin C treatment in the LOVIT trial, with heterogeneity of treatment effect in the magnitude of harm. Trial registration: Funded by the Lotte and John Hecht Memorial Foundation; LOVIT ClinicalTrials.gov number, NCT03680274.
KW - Ascorbic acid
KW - Cluster analysis
KW - Cytokines
KW - Precision medicine
KW - Sepsis
KW - Subphenotype
KW - Subtype
U2 - 10.1007/s00134-024-07733-9
DO - 10.1007/s00134-024-07733-9
M3 - Article
SN - 0342-4642
JO - Intensive Care Medicine
JF - Intensive Care Medicine
M1 - e33989
ER -