Head & neck squamous cell carcinoma: Comparison of multimodal imaging with pathological specimens
Emmanouil Terzidis,
Sweden
PD-0821
Abstract
Head & neck squamous cell carcinoma: Comparison of multimodal imaging with pathological specimens
Authors: Emmanouil Terzidis1, Jeppe Friborg1, Anders B Olin2, Ivan R Vogelius1, Giedrius Lelkaitis3, Christian Buchwald4, Helle H Johanesen2, Barbara Malene Fischer2, Irene Wessel4, Jacob H Rasmussen4
1Rigshospitalet, Department of Oncology, section of Radiotherapy, Copenhagen, Denmark; 2Rigshospitalet, Department of Clinical Physiology & Nuclear Medicine, Copenhagen, Denmark; 3Rigshospitalet, Department of Pathology, Copenhagen, Denmark; 4Rigshospitalet, Department of Otorhinolaryngology, Head & Neck Surgery and Audiology, Copenhagen, Denmark
Show Affiliations
Hide Affiliations
Purpose or Objective
Despite development in imaging modalities, precise target definition
remains a major challenge in head and neck cancer. In this study, tumor volumes
defined from multimodal imaging with PET/MRI prior to surgery are compared with
the actual pathological tumor volumes from surgical specimens. The mismatch between
the volumes defined from imaging and pathology is estimated and the clinical
impact of potential mismatch is evaluated.
Material and Methods
Twenty-eight patients with head and neck squamous cell carcinoma were scanned on an integrated PET/MRI system, prior to surgery. Three GTV’s were delineated defined from the MRI (GTVMRI), the PET (GTVPET) and one by utilizing both anatomical images and clinical information (GTVONCO). Surgical specimens were extracted en bloc and scanned with the same PET/MRI and co-registered to the patient images based on predefined anatomical landmarks. Each specimen was sectioned in blocks which were then sliced (4-µm thick) and stained with haematoxylin and eosin. All slices were digitalized, scanned and pathological tumor volume was delineated by a trained head and neck pathologist. Pathological tumor areas were interpolated to yield a 3D tumor volume (GTVPATO), which was imported in Eclipse TPS (Varian Medical Systems, Palo Alto, CA) as a structure. The GTVPATO was compared with the GTV’s defined from imaging. Additionally, the mismatch between GTV’s were assessed by dividing the GTVPATO that is outside the imaging GTV with the whole volume of the corresponding GTV. To validate current practice of a 5 mm CTV expansion, a margin of 5 mm was added to the GTVONCO and the mismatch was re-assessed.
Results
For consistency, only T-sites were included in this analysis (N=27). Further
thirteen patients were excluded before the analysis, because fragmentation of
the specimen during histologic processing or poor interpolation and insufficient
number of points to form a structure in Eclipse. For the fourteen patients that
were included in the analysis the mean volume of the GTVONCO was
larger than the other GTV’s. In four patients the GTVPATO was larger
than the GTVMRI and for one patient the GTVPATO was larger
than the GTVPET. The mean mismatch of the GTVPATO when
evaluated to the GTVPET, GTVMRI and GTVONCO was
29.7%, 39.5% and 7.5% respectively (Table 1). However, after the addition of
5mm margin all GTVPATO’s
were encompassed in GTVONCO.
Conclusion
GTV was defined differently with different imaging
modalities and a mismatch with the pathological tumor volume was observed in
thirteen of the fourteen included patients. For all patients, 5mm margin appears sufficient to ensure
that all of the pathological information will be included during treatment.