Introduction
Treatment for advanced colorectal cancer (CRC) has evolved over the
years, particularly recently with the addition of novel targeted agents
to chemotherapy. There are now several treatment combinations and
treatment sequences from which patients can benefit under a continuum of
care. This case describes a patient with metastatic CRC (mCRC) who
initially received upfront capecitabine-oxaliplatin with bevacizumab.
Due to poor disease response, she was switched to another cytotoxic
combination with a targeted agent and has demonstrated a response.
Presentation and disease course
The patient is a 63-year-old female, with good functional status, who
presented to the clinic in February 2014 with right upper quadrant pain.
Upon further investigation, she was found to have stage IV CRC with
multiple metastatic liver lesions. The tumour tested positive for KRAS
mutation. At the time of diagnosis, the tumour was deemed unsuitable for
resection and, consequently, the patient was offered combination
cytotoxic chemotherapy with the targeted biological agent bevacizumab.
The patient initially requested foregoing bevacizumab treatment to avoid
the potential side effect of bleeding. She also requested foregoing a
convenient regimen and consequently underwent three cycles of
capecitabine with oxaliplatin, or XELOX (capecitabine, 1,400 mg twice a
day from days 1 to 14; oxaliplatin, 170 mg given every 3 weeks) as an
outpatient.
A follow-up positron emission tomography-computed tomography (PET-CT)
scan showed only minimal tumour response (Figure), and her
carcinoembryonic antigen (CEA) level had increased from the pretreatment
level of 130 ng/mL to 190 ng/mL. The patient agreed to add bevacizumab
(350 mg/cycle, given every 3 weeks) to XELOX at the fourth cycle. After a
total of six cycles of XELOX, however, only a small decrease in CEA was
seen, Second-line treatment options with other chemotherapy
combinations were discussed with the patient, and she continued to
stipulate a preference for outpatient treatment. From July 2014, the
patient received irinotecan (260 mg) with the addition of the targeted
agent aflibercept (200 mg/cycle, given every 2 weeks) to optimize tumour
response. Capecitabine was not used because she had thrombocytopenia
during the XELOX regimen.
The CEA level decreased to 30 ng/mL at the third cycle of second-line
therapy, and to 13.3 ng/mL after the sixth cycle. Furthermore, following
the sixth cycle, her tumour responded with marked decrease in size and
in fluorodeoxyglucose (FDG)uptake of liver lesions (Figure). The patient
developed neutropenia (but no fever); otherwise, she tolerated her
treatment well. She had earlier received granulocyte colony-stimulating
factor (G-CSF) for chemotherapy support.
........cont'
Reference information: www.cancerdoctor.hk
The information aims to provide educational purpose only. Anyone reading
it should consult Oncologist before considering treatment and should
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