Superficial wIRA-hyperthermia and re-irradiation: Role of oxygen-dependent radiosensitization
PD-0490
Abstract
Superficial wIRA-hyperthermia and re-irradiation: Role of oxygen-dependent radiosensitization
Authors: Andreas Thomsen1, Michael R. Saalmann1, Markus Notter2, Nils H. Nicolay1, Anca-L. Grosu1, Peter Vaupel1
1University Medical Center, University of Freiburg, Radiation Oncology, Freiburg, Germany; 2Lindenhofspital, Radiation Oncology, Bern, Switzerland
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Purpose or Objective
The treatment of unresectable local recurrences
of superficial tumors in pre-irradiated areas is a major challenge when the
option of re-irradiation (re-RT) using standard dose is questionable due to
expected unacceptable toxicity.
A novel treatment protocol of contact-free
thermography-controlled superficial hyperthermia (HT) using water-filtered
infrared-A (wIRA) irradiation immediately followed by hypofractionated re-RT of
20 Gy total dose (5 x 4 Gy, 1x/week) has shown a most favorable toxicity/efficacy
profile in the treatment of large-sized, locally recurrent breast cancer (Notter
et al., Cancers 2020).
Different (radio-)sensitizing mechanisms of HT require
different temperature ranges. Whereas the inhibition of DNA repair requires HT-levels
≥41.5°C, O2-dependent mechanisms can already operate at ≥39°C, and may be
counteracted at temperatures ≥43°C. Using mild HT immediately before re-RT, O2-dependent
radiosensitizing mechanisms thus may play a key role.
Material and Methods
Experiments on healthy
volunteers were performed using the wIRA-hyperthermia system hydrosun®TWH1500
(Hydrosun, Germany) with approval of the local ethics committee. At
automatically controlled maximum skin surface temperatures of 43°C, temperature
profiles within the abdominal wall were measured with fiber optic sensors
(OTG-M600, Opsens, Canada) at defined tissue depths of 1-20 mm. Corresponding
pO2 values were assessed with the OxyLite-Pro system (Oxford
Optronix, UK). Hyperspectral tissue imaging (TIVITA, Diaspective Vision,
Germany) was used to visualize the HbO2- oxygenation status of upper
skin layers, and of superficial tumors in selected patients.
Results
Within 5-12 min of
wIRA-exposure, mean skin surface temperatures increased from 34.6 to 41.6°C.
Upon steady state conditions, mean maximum temperatures of 41.8°C were found at
a tissue depth of 1 mm, with a steady decline in deeper layers (41.6°C @ 5 mm,
40.8°C @ 10 mm, 40.6°C @ 15 mm, 40.1°C @ 20 mm). Tissue heating was accompanied
by a significant increase in tissue pO2, e.g., at a depth of 13 mm
mean pO2 rose from 46 to 81 mmHg. In the post-heating phase (+15
min), pO2 was still elevated (72 mmHg), even though tissue
temperatures had returned to normothermia (36.7°C). pO2 values
remained above baseline for 30-60 min post-heat. Non-invasive HbO2 monitoring
in the subpapillary dermis layer of normal skin and in recurrent breast cancers
confirmed the improved O2 status caused by wIRA-HT.
Conclusion
wIRA-hyperthermia (T =
39-43°C) leads to a distinct pO2 rise in superficial tissues, which
is essential for radiosensitization. This benefit of improved tissue
oxygenation is only present if HT is applied shortly before radiotherapy.
Effective HT levels needed for inhibition of DNA repair could be observed up to
a tissue depth of ≈5 mm, as present, e.g., in lymphangiosis carcinomatosa. Effective
HT levels for improved oxygenation (T ≥ 39°C) can be measured up to a tissue depth
of ≈30 mm.