Rectal Cancer Clinical Trial
Official title:
The Value of PET / MRI for the Assessment of Lymph Node Metastasis and Other Prognostic Factors in Patients With Rectal Cancer
The combination of FDG-PET/CT and MRI at staging of rectal cancer in diagnosis is currently
very little studied. The investigator have a unique opportunity to study this.
Hypothetically, with PET/MR as one hybrid imaging method, alternatively as an additional
method, it could increase the accuracy of rectal cancer of moderate and high risk type,
especially at primary N-staging, but also in assessing other important prognostic factors
such as T-staging, peritoneal involvement, metastasis to lateral lymph nodes, EMVI and MRF
involvement. The same reasoning applies to the assessment of tumor regression after CRT.
In the study, PET/MR is compared with PET/CT, diagnostic CT and MRI to evaluate the
additional value of the hybrid imaging PET/MRI. The investigator also plan to evaluate how
immunological, proliferative and prognostic biomarkers in blood and tumor tissue correlate
with the radiological findings, and if the combination biomarker and radiology can provide
additional prognostic information.
Today, there is a variety of treatment options in diagnosed rectal cancer. The standard
treatment is surgery with removal of the tumour including surrounding fat and lymph nodes in
a package. Prior to surgery, the patient may be given a shorter or longer radiation
treatment, the latter in combination with cytostatics, depending on staging at the time of
diagnosis. Cytostatic drugs can also be given post surgery. The choice of treatment for the
individual patient is based on the assessment of the imaging, ie conventional X-ray,
ultrasound, computed tomography, (CT), Magnet Resonance Tomography Imaging (MRI) and Positron
Emission Tomography in combination with CT (PET/CT). An accurate staging assessment is
crucial for adequate treatment of rectal cancer patients to avoid over treatment, which in
itself causes unnecessary suffering, or under treatment with increased risk of relapse. With
today's methods, tumor size, overgrowth of other organs and spread to other organs such as
liver and lung can be reasonable assessed. On the other hand, there is great uncertainty when
assessing spread to lymph nodes. Better safety is also needed for other prognostically
important factors such as tumor involvement of the mesorectal fasciae (MRF), i.e. the rectum
surrounding the tumor, and tumor growth in venous vessels outside the intramural invasion of
the intestinal wall, EMVI.
Hybrid imaging with PET combined with magnetic resonance imaging (PET/MR) is a novel method
and there are currently no published studies comparing the outcome of fluoro-deoxy glucose
(FDG) -PET/MR with CT, MR, PET/CT at staging of rectal cancer, both primarily and after
radiation and cytostatics treatment (CRT). In this study, the investigator plan to evaluate
the additional value for PET/MR in rectal cancer. Only patients to be operated are included
and microscopic examination of the preparation, histopathology, will be the reference method
with which survey data from the imaging methods are compared. The investigator also want to
evaluate the relationship between the radiological findings and biomarkers in blood and tumor
tissue to determine if there is a relationship that can provide additional prognostic
information. The investigator will only include patients with intermediate and high-risk
rectal cancer, as low-risk cancer is unusual with spread to lymph nodes. The study will be a
prospective observation study in which all consecutive elective patients in Umeå with
confirmed intermediate and high risk type rectal cancer, which give their consent, are
included and examined preoperatively. Thereafter, imaging and blood and tumor tissue samples
are examined and evaluated.
Primary research questions:
- Can FDG-PET/MR provide improved accuracy in assessment of local tumor proliferation,
lymph node metastasis and other important prognostic factors (MRF +, EMVI) in rectal
cancer compared to currently used methods magnetic resonance imaging, (MRI), PET/CT or
CT?
- Can FDG-PET/MR provide an improved accuracy in assessment of tumor regression following
combined cytostatics and radiotherapy in rectal cancer compared to MRI or PET/CT?
- Can FDG-PET / MR in combination with blood and tumor tissue biomarkers provide
additional prognostic information for intermediate and high-risk rectal cancer?
Secondary research questions:
• How does the accumulation of FDG change in rectal cancer tissue when examined after 60
minutes vs examination after 90 minutes?
Patients will be examined with a whole body FDG-PET CT, where the CT replaces the regular
diagnostic CT examination. There is also a FDG-PET/MR of the pelvic region, where the MR part
replaces the regular MRI examination. For patients with locally advanced disease undergoing
combined radiation and chemotherapy, a further PET/CT and PET/MR are acquired at least 4
weeks after the treatment, but before surgery. In future, patients who only need shorter
radiation therapy may undergo further PET/CT and PET/MR before surgery, if time between
radiation and surgery is extended as clinical routine.
PET/CT and PET/MR are done immediately after each other with only one FDG injection of 4
Mbq/kg body weight. The examinations will be reviewed and judged according to clinical
routine, where all reviewers have access to all image data. An additional reading will then
be done by experienced GI-radiologist and nuclear medicine physician to assess the additional
value for PET/MR. The histopathological finding in the examination of the surgical
preparation will be used as a reference method.
In order to facilitate the assessment and correlation between individual lymph nodes in
tissue analysis and imaging data, the operation specimen will, when this is possible, be
examined with MRI postoperatively before the histopathological examination is performed.
The study does not involve any extra visits in addition to clinical routine at the Department
of Radiology, but gives a small increase in radiation dose, as PET/MR is done instead of MRI
only and in addition to PET/CT after CRT, which is not clinical routine. According to
national guidelines, PET/CT is intended for advanced rectal cancer, but for those not
included in this group, there will be an increased radiation dose of PET in PET/CT. This
increase of ionizing radiation is small and corresponds to approximately 2 years of
background radiation.
Radiological image data (PET/MR and PET/CT) is stored in the picture archiving and
communicating system (PACS) as in clinical routine. Requests and reports are stored in the
Department's Radiological Information System (RIS).
The examination is subject to the same confidentiality as any routine imaging examination at
the department. Image data will not be destroyed. Data is exported to external software for
post processing and statistical processing. All processing in addition to clinical routine
takes place in unidentified data. Only those responsible and employees in the project have
access to conversion lists.
The primary objective of this study is assessment of lymph node metastases. The best method
today is MR which has a sensitivity of 77% and a specificity of 71%. With an estimated 20%
prevalence of lymphoma metastases, an expected sensitivity of 90%, an expected specificity of
80% and 80% statistical strength, and 95% confidence interval, 307 glands are required for
sensitivity and 691 glands for specificity. As the investigator expect to identify 8 glands
per patient, it means that about 39 patients is needed for the sensitivity and about 87
patients for the specificity. The investigator round up the number of patients to 100 to
compensate for any failure in the follow-up.
Written information is provided to the patient and patient leaves his signature. All signed
consent is given to the x-ray department where they are filed at the research department.
Individuals who can not or do not want to give consent are not included. This also applies to
individuals with reduced decision-making skills.
The examination is subject to the same confidentiality as any routine x-ray examination at
the clinic. Evaluation of the find takes place under safe forms within a limited circle and
data is kept in safe storage. If external statistical consultation is required, patient data
will be unidentified.
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