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Recombinant Human Tissue Kallikrein-1 for Treating Acute Ischemic Stroke and Preventing Recurrence

  • Scott E. Kasner*
  • , Philip M. Bath
  • , Michael D. Hill
  • , John J. Volpi
  • , Michael Giuffre
  • , Lorianne Masuoka
  • , David Wambeke
  • , Paolo R. Madeddu
  • *Autor correspondiente de este trabajo
  • University of Pennsylvania
  • University of Nottingham
  • University of Calgary
  • Houston Methodist
  • University of Calgary
  • DiaMedica Therapeutics
  • University of Bristol

Producción científica: Contribución a una revistaArtículo de revisiónrevisión exhaustiva

6 Citas (Scopus)

Resumen

Novel strategies are needed for the treatment of acute ischemic stroke when revascularization therapies are not clinically appropriate or are unsuccessful. rKLK1 (recombinant human tissue kallikrein-1), a bradykinin-producing enzyme, offers a promising potential solution. In animal studies of acute stroke, there is a marked 36-fold increase in bradykinin B2 receptor on brain endothelial cells of the ischemic region. Due to this environment, rKLK1-generated bradykinin will exert a potent local vasodilation and increase brain perfusion via 3 synergistic signaling pathways downstream to the B2 receptor. Because of its preferential effect on ischemic tissue, systemic adverse effects such as hypotension are avoided with proper dosing. In addition, with initial vasodilation through recruitment of preexisting collaterals, rKLK1 promotes long-term benefit of brain perfusion by promoting new collateral formation. With an extended course of therapy for weeks after acute ischemic stroke, these multifaceted effects may also reduce the risk of stroke recurrence. A prior phase II trial demonstrated a favorable impact on clinical outcomes and recurrent strokes, particularly among patients who were not eligible for mechanical thrombectomy. A phase II/III trial has launched in this population, though opportunities for combination revascularization therapies deserve further investigation.

Idioma originalInglés
Páginas (desde-hasta)745-753
Número de páginas9
PublicaciónStroke
Volumen56
N.º3
DOI
EstadoPublicada - 1 mar. 2025
Publicado de forma externa

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