Your search keyword '"Stover, Brian"' showing total 2 results

1. mRNA aggregates harness danger response for potent cancer immunotherapy

Author

Mendez-Gomez, Hector R., DeVries, Anna, Castillo, Paul, Stover, Brian D., Qdaisat, Sadeem, Von Roemeling, Christina, Ogando-Rivas, Elizabeth, Weidert, Frances, McGuiness, James, Zhang, Dingpeng, Chung, Michael C., Li, Derek, Zhang, Chong, Marconi, Christiano, Campaneria, Yodarlynis, Chardon-Robles, Jonathan, Grippin, Adam, Karachi, Aida, Thomas, Nagheme, Huang, Jianping, Milner, Rowan, Sahay, Bikash, Sawyer, W. Gregory, Ligon, John A., Silver, Natalie, Simon, Eugenio, Cleaver, Brian, Wynne, Kristine, Hodik, Marcia, Molinaro, Anette, Guan, Juan, Kellish, Patrick, Doty, Andria, Lee, Ji-Hyun, Carrera-Justiz, Sheila, Rahman, Maryam, Gatica, Sebastian, Mueller, Sabine, Prados, Michael, Ghiaseddin, Ashley, Mitchell, Duane A., and Sayour, Elias J.

Subjects

Article

Abstract

Messenger RNA (mRNA) has emerged as a remarkable tool for COVID-19 prevention but its use for induction of therapeutic cancer immunotherapy remains limited by poor antigenicity and a regulatory tumor microenvironment (TME). Herein, we develop a facile approach for substantially enhancing immunogenicity of tumor-derived mRNA in lipid-particle (LP) delivery systems. By using mRNA as a molecular bridge with ultrapure liposomes and foregoing helper lipids, we promote the formation of ‘onion-like’ multi-lamellar RNA-LP aggregates (LPA). Intravenous administration of RNA-LPAs mimics infectious emboli and elicits massive DC/T cell mobilization into lymphoid tissues provoking cancer immunogenicity and mediating rejection of both early and late-stage murine tumor models. Unlike current mRNA vaccine designs that rely on payload packaging into nanoparticle cores for toll-like receptor engagement, RNA-LPAs stimulate intracellular pathogen recognition receptors (RIG-I) and reprogram the TME thus enabling therapeutic T cell activity. RNA-LPAs were safe in acute/chronic murine GLP toxicology studies and immunologically active in client-owned canines with terminal gliomas. In an early phase first-in-human trial for patients with glioblastoma, we show that RNA-LPAs encoding for tumor-associated antigens elicit rapid induction of pro-inflammatory cytokines, mobilization/activation of monocytes and lymphocytes, and expansion of antigen-specific T cell immunity. These data support the use of RNA-LPAs as novel tools to elicit and sustain immune responses against poorly immunogenic tumors.

Published

2023

2. A Prospective Study of Negative Pressure Wound Therapy With Integrated Irrigation for the Treatment of Diabetic Foot Ulcers

Author

Zelen, Charles M., Stover, Brian, Nielson, David, and Cunningham, Muriel

Subjects

integumentary system, Journal Article

Abstract

Objective: Patients with diabetes often present with pedal wounds resistant to standard wound healing modalities and become chronic in nature. These chronic wounds in diabetic patients have a high incidence of complications including infection and amputation. Negative pressure wound therapy has been found to facilitate healing of the stagnant pedal wound. This protocol was designed to determine wound closure rates using a unique negative pressure wound therapy system that delivers vacuum-assisted wound closure with a simultaneous irrigation feature (Svedman Wound Treatment System). Methods: A prospective single center study was conducted in adults with diabetic foot ulcers ≥cm2 or more in size showing no signs of clinical infection, and having adequate blood flow. Patients received dressing changes and irrigation on a standard regimen with weekly wound assessments for a minimum of 6 weeks. Results: 11 women and 8 men with a mean wound size of 2.4 cm × 2.2 cm were treated with the device. A total of 14 of /19 (74%) patients healed completely, with a median healing time of 34 days (range, 9-114). Eleven of 19 patients (58%) healed within the 6-week evaluation period. For the 5 patients who did not heal completely with the device, other treatments were utilized, including further wound debridement, muscle flaps, and skin grafting procedures. Conclusions: Negative pressure wound therapy with integrated irrigation was well tolerated by the patients without complications related to the device application or irrigation feature. The data clearly suggests that this technology may be a promising alternative for the chronic nonhealing diabetic wound.

Published

2011