Cholangiocarcinoma Clinical Trial
Official title:
International Registry on Cholangiocarcinoma Treatment
Cholangiocarcinoma is a rare and very aggressive neoplasm that arises from the biliary
epithelium, constitutes approximately 2% of all reported cancer, and accounts for about 3% of
all gastrointestinal malignancies. Up to date, there are many modalities to diagnosis and
treat with a range of sensitivity and specificity, and also the advantage and disadvantage of
its modality. Cholangiocarcinoma has a poor prognosis. Surgical resection offers the only
curative option and usually requires a major hepatic resection in addition to resection of
the cholangiocarcinoma. Unfortunately, curative resection is possible in only about 30% of
patients due to locally advanced disease, distant metastases or comorbidity in elderly
patients. Even after resection, the recurrence rate is approximately 60%, resulting in a low
5-year overall survival (OS).
Patients with intra-hepatic Cholangiocarcinoma (ICC) have a very limited benefit from
systemic chemotherapy, indeed, in unresectable cholangiocarcinoma Overall Survival with
systemic chemotherapy is less than 1 year. Since most cholangiocarcinoma patients develop
distant metastases at late stages only, locoregional therapy is an interesting therapeutic
strategy.
Locoregional therapy studies in patients with intrahepatic cholangiocarcinoma employing
radiofrequency ablation (RFA), transarterial chemoembolization (TACE) or external as well as
internal radiation therapy yielded promising results in the last couple of years.
TACE is safe and may be effective for prolonging the survival of patients with nonresectable
combined hepatocellular carcinoma (HCC) -cholangiocarcinoma, as compared with the
historically reported survivals of these patients. Tumor vascularity is highly associated
with tumor response. The patient survival period after TACE for combined
HCC-cholangiocarcinoma is significantly dependent on tumor size, tumor vascularity,
Child-Pugh class, and presence or absence of portal vein invasion.
Currently, few centers perform TACE therapy for unresectable Cholangiocarcinoma. Several
European studies have reported the efficacy and safety TACE for ICC.
The establishment of a registry to obtain the majority of Cholangiocarcinoma cases treated
with locoregional approach within and outside Europe can help the investigators evaluate a
larger and non-ambiguous sample population. This would help the investigators evaluate the
technical success rates, clinical success rates, feasibility and safety of TACE for ICC.
Study Design: Prospective observational study
Primary objective: This is a data collection study where the main purpose is to collect
information about the treatments that patients receive for their unresectable
cholangiocarcinoma.
Secondary objectives: To create an international Registry including patients undergoing
locoregional treatments, to correlate tumour characteristics with outcome, survival and
prognosis; to identify criteria for guiding therapy including TACE, chemoinfusion and other
locoregional treatments
Treatment modalities for TACE
Day -1 Doxorubicina 50-75 mg/mq has been charged onto 2 ml of 70-150 µm M1 microspheres at
Pharmacy.
Day -1 : prehydration, antibiotic prophylaxis and setting up of a therapeutic scheme
appropriate for analgesic prophylaxis (3-day duration) as previously reported 1 vial of
tropisetron (diluted in 100ml of physiological solution) administered by slow drip Day 0:
Upon admittance to the radiology room, the patient receive morphine hydrochloride 10 mgr
diluted in 100 ml of salin solution i.v. (to be repeated one hour after the procedure and if
necessary also after 6 hours).
Tropisetron i.v. if needed. Intra-arterial premedication with 2.5 mgr of verapamil 2.5 mgr
diluted in 4 ml of normal saline solution followed by 4 ml of lidocaine 2%.
Selected arterial Infusion (considering tumor uptake and dominant disease) of doxorubicina
50-75 mg preloaded into 2 ml of 70-150 µm M1 microspheres.
Second infusion of doxorubicin at the same dose into 2 ml of 70-150 µm M1 microspheres can be
administered in a further TACE (oncologist's planning of cure).
Day +30: The above procedure is repeated. Day +90: In case of response, a third
administration following the above procedures will be repeated
Evaluation of response
Response must be assessed by repeating the following examinations at Day 30, Day 90 and Day
120 after start of treatment:
Chest-abdomen CAT scan with and without contrast medium (refer to Section 4). Evaluation will
be based on the Response Evaluation Criteria In Solid Tumors (RECIST) cancer markers (CEA),
Cancer Antigen (CA) 19.9)
Assessment of quality of life The Edmonton Symptom Assessment System (ESAS) is used to
monitor health conditions and quality of life.
The questionnaire must be filled in by the patient unaided by family members or by health
care personnel, over a period of about 15 minutes. Assessment of quality of life will be
performed during the baseline visit and at Day 30, Day 60 and Day 120 from start of
treatment.
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