par Vincent, Jean Louis 
;van der Poll, Tom;Marshall, John C
Référence Biomedicines, 10, 9, 2260
Publication Publié, 2022-09
;van der Poll, Tom;Marshall, John CRéférence Biomedicines, 10, 9, 2260
Publication Publié, 2022-09
Article révisé par les pairs
| Résumé : | Sepsis, defined as life-threatening organ dysfunction caused by a dysregulated host response to an infection, remains a major challenge for clinicians and trialists. Despite decades of research and multiple randomized clinical trials, a specific therapeutic for sepsis is not available. The evaluation of therapeutics targeting components of host response anomalies in patients with sepsis has been complicated by the inability to identify those in this very heterogeneous population who are more likely to benefit from a specific intervention. Additionally, multiple and diverse host response aberrations often co-exist in sepsis, and knowledge of which dysregulated biological organ system or pathway drives sepsis-induced pathology in an individual patient is limited, further complicating the development of effective therapies. Here, we discuss the drawbacks of previous attempts to develop sepsis therapeutics and delineate a future wherein interventions will be based on the host response profile of a patient. |
