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Profound immune suppression, including conditions such as anergy, secondary immune suppression, and immune exhaustion, severely disrupts immune surveillance in preclinical models such as animals with tumors, sepsis, or chronic viral infections. This hypothesis presents an innovative experimental framework designed to stimulate localized immune signaling by mimicking physiological signals using precise, controlled-dose mechanisms. Proposed strategies include molecular triggers derived from parasites (e.g., ectoparasite saliva components and phospholipase), mild metabolic stress induced by subtoxic ethanol, and sensory activation of immunity through peripheral electrical stimulation. These approaches aim to selectively enhance local immune responses while preventing systemic activation, exploiting synergistic interactions between innate and adaptive immunity. All concepts are theoretical and require thorough testing in vitro and in vivo, with potential risks including allergic reactions and cytotoxicity. No therapeutic claims are made.

Disclaimer:The following approaches represent theoretical experimental models aimed at initiatinglocal immune signaling under conditions of profound immune suppression. These conceptsare not intended as therapeutic recommendations and are not validated for clinicalapplication. All proposed mechanisms require rigorous in vitro and in vivo evaluation.Potential risks include allergic reactions, cytotoxicity, and other immunological orphysiological side effects. Application outside controlled laboratory research is stronglydiscouraged.