More than 6000 people in Sweden are diagnosed with colorectal cancer annually. One out of
five patients already has metastases at diagnosis. However, the occurrences of metastases at
specific locations, e.g. peritoneal carcinomatosis and ovarian metastases, are not well known.
The development of surgical and oncological treatment strategies for primary tumours and
metastatic disease has led to a need to discuss colorectal cancer patients in a multidisciplinary
team (MDT). Although oncologic cure and overall survival are the main goals of treatment,
quality of life and functional results are becoming increasingly important with the prolonged
survival. While male sexual dysfunction after rectal cancer treatment has been well described,
considerably less data have been published about the impact on women. In addition to surgical
trauma, female androgen insufficiency could be a contributing factor to sexual dysfunction.
Radiotherapy for rectal cancer may increase the risk of reduced ovarian androgen production,
but there is scant information on this in the literature.
Papers I-III are large population-based cohort studies reporting on the effects of the development
and implementation of MDT-conferences in patients with metastatic disease (Paper I)
and the epidemiology of peritoneal carcinomatosis and ovarian metastases in colorectal cancer
patients (Papers II–III). MDT assessment and metastasis surgery were more common in rectal
cancer patients than in colon cancer patients, and the proportion increased over time. Peritoneal
carcinomatosis was common, and risk factors were colon cancer, advanced tumour and nodal
stage, fewer than 12 examined lymph nodes, emergency surgery, and a non-radical resection of
the primary tumour. Ovarian metastases were uncommon, especially in rectal cancer patients.
Paper IV assesses feasibility and internal and external validity in a prospective, observational
cohort study on sexual function and androgen levels in women with rectal cancer. The methods
were workable and the patients’ compliance was good. Comparison of clinical data from the
study cohort with that of women who were eligible for inclusion but not included revealed a
selection bias. Having a partner and sexual activity was more common among women who
answered all questions in the questionnaires about sexual function compared with those who
did not. A power calculation based on data from the first included patients showed that a larger
sample size than initially planned for was needed.
In conclusion, an increasing proportion of patients with metastatic colorectal cancer were discussed
by the MDT. Predictors for and the occurrence of peritoneal carcinomatosis and ovarian
metastases were defined, which may help to decide on individual treatment and follow-up
regimens. The analysis of baseline data from the study on sexual function and androgen levels
in women with rectal cancer indicates feasible methods but a selection bias. Inclusion of new
patients in the study continues