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Gezond weefsel beter sparen Dat is het voordeel van protonentherapie.

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Waarom protonentherapie Algemene informatie Soorten kanker Ervaringen van patiënten Tips en adviezen Second opinion Jongvolwassen en kanker Lopende studies
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Research

Research

How HollandPTC works to enhance the benefits of proton therapy

 

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HollandPTC

HollandPTC

Voor de beste protonentherapie van nu en later

Over HollandPTC
Onze visie: Samen beter, beter samen Ons team HollandPTC software
Vrienden van Cliëntenraad Diversiteit en gelijkheid

SAMEN BETER, BETER SAMEN

Patiënten

Patientenzorg

Gezond weefsel beter sparen Dat is het voordeel van protonentherapie.

Bekijk
Over de behandeling Waarom protonentherapie Algemene informatie Soorten kanker Ervaringen van patiënten Tips en adviezen Second opinion Jongvolwassen en kanker Lopende studies
Uw bezoek aan HollandPTC Locatie en contactgegevens Wat neemt u mee Vervoer en overnachten Compliment of klacht
Praktische informatie Vergoeding van uw behandeling Uw dossier
Research

Research

How HollandPTC works to enhance the benefits of proton therapy

 

View
Research at HollandPTC Our principal investigators Organisations & collaborations Research projects
Facilities Pre-clinical and clinical facilities Our research database: how to request data Doing proton research or use our facilities
Practical information Practical information on Varian projects R&D communication box Contact
HollandPTC

HollandPTC

Voor de beste protonentherapie van nu en later

Over HollandPTC
Over HollandPTC Onze visie: Samen beter, beter samen Ons team HollandPTC software
Vrienden van Cliëntenraad Diversiteit en gelijkheid

Protect – proton versus photon therapy for esophageal Cancer

Principal Investigatorsprof. dr. Mischa Hoogeman (HollandPTC and dr Hedwig Blommestein (HollandPTC)

 PhD students: Quais Akolawala (TU Delft)

Funding: TU Delft Health Initiative 2022

Description

The development of physiological engineered in vitro models assumes a pivotal role in the understanding and treatment of diseases. Among these, glioblastoma is the most aggressive type of brain cancer with a yearly incidence of 3 cases per 100,000 people. Prospects for patients are bleak, with a median survival of just 15 months after diagnosis despite chemoand radiotherapy. An alternative promising solution is proton therapy, which is able to offer effective treatment with less radiation exposure to the brain. In particular, FLASH proton therapy, compared to conventional dose-rate irradiation, is 400-fold more rapid (≥ 40 Gy/s), thus further reducing the damage to healthy tissue and shortening treatment time. However, systematic in vivo studies of the effect of FLASH proton therapy on glioblastoma are lacking, as are reliable in vitro platforms to assess dose efficiency. This is because investigations on the morphological and functional changes of cells after being exposed, cannot be routinely performed on patients or tissues coming from biopsies. On the other hand, in vitro studies of cells mostly rely on strategies that do not realistically represent the three-dimensional (3D) spatial configuration in our brain.

There is therefore an urgent need for 3D cell-instructive microenvironments that can be (1) exploited as standardized and biomimetic in vitro models for understanding how the third dimension affects brain cancer cell development, and (2) used as a platform to assess FLASH therapy. The development of reliable 3D organ-on-chip devices is of central interest for the Netherlands’ Top Sector “Life Science and Health”. Current approaches include, however, either 3D microenvironments or microfluidic devices; a platform embedding both features is still missing. To fill this gap, we propose to realize a standardized, reproducible, and physiologically relevant 3D glioblastoma organ-on-chip and use it for assessing the effect of FLASH protontherapy.