Cervical Cancer Clinical Trial
Official title:
A Prospective Study on the Efficacy and Safety of the Re-irradiation of Recurrent Cervical Cancer Within the Irradiated Field by Intensity Modulated Radiotherapy
this is a prospective clinical trial using intensity modulated radiotherapy(IMRT)for the treatment of cervical cancer patients with recurrent disease within the previously irradiated field. Sixty patients will be enrolled after careful selection to meet the including criteria and excluding criteria. A primary course of 36Gy will be prescribed to the recurrent site and a further 9-24Gy of dose escalation will be prescribed to the gross tumor volume in the second course according to the toxicities and the shrinkage of tumor. Weekly concurrent cisplatin of 30mg/m2 by five weeks will be administrated intravenously to the selected patients. Acute and late toxicities will be monitored and survival endpoints will be tracked with our follow-up protocol to evaluate the safety and efficacy of this approach.
Introduction: Cervical cancer is the seventh most common and the eighth deadliest cancer in
Chinese women. In spite of the advances in multimodality treatment regimens, there were
15-40% patients suffering from recurrence within initial irradiated field[1, 2], of which 95%
recurrence occurred within 2 years and only 20% of them could be treated by salvage
treatment[3-6]. there were controversies on how recurrent cervical cancer within the
irradiated field should be dealt with. Surgery such as pelvic extenteration had to remove
involved organs including intestine, rectum or bladder and sometimes led to severe
complications and a poor quality of life. After the initial 45-50Gy irradiated to the whole
pelvis, it seemed to have minimal space of further re-irradiation for recurrent disease as
conventional radiotherapy was applied when considering late toxicities of organs at risk. The
radiation dose for pelvic structures received will reach 45-50 Gy, almost reached the upper
limits of normal tissues. For recurrent cervical cancer patients receiving retreatment by
radiotherapy, the toxicity increased by 30%-56%[2] when conventional technique was applied,
toxicities restricted sufficient treatments to the recurrence disease leading to a poor
prognosis, which was usually less than a year [8]. IMRT has an advantage over conventional
techniques because of delivering a high dose to target volume while sparing organs at risk
which were previously irradiated in the primary radiotherapy. We have a five years'
experience using IMRT to treat patients with recurrent disease within the previously
irradiated field and most of patients showed good response and tolerable complication.
According to our retrospective research (publishing), thirty-three patients made a median
survival time of 14.06 months, one year overall survival was 55% and 2 year overall survival
was 22%, which were better than the results of one year survival 10-20% from previous studies
[8]. For further evidence, we designed this prospective clinical trial to evaluate the
efficacy and safety when using intensity modulated radiotherapy to treat patients with
recurrent cervical cancer within the previously irradiated field.
Methods: Sixty patients with recurrent cervical cancer within the previously irradiated field
will be prospectively enrolled in this study. Only patients meeting both the including
criteria and exclusion criteria will be carefully selected considering potential severe
toxicities. A primary course of 36Gy will be prescribed to the recurrent site and a further
9-24Gy of dose escalation will be prescribed to the gross tumor volume in the second course
according to the toxicities and the shrinkage of tumor to the irradiation. Intensity
Modulated RadioTherapy (IMRT) will be chosen for dose delivery as this technique gives
sufficient dose to target volume meanwhile sparing organs at risk. Weekly cisplatin of
30mg/m2 by five weeks will be administrated intravenously to the selected patients.
Outcome measurements: Toxicities will evaluated using Common Terminology Criteria for Adverse
Events version 4.0 (CTCAE 4.0). Acute toxicities will be monitored weekly until one month
after the completion of radiotherapy and chemotherapy. Then late toxicities will be recorded
by monthly following-up. Three year's progression free survival (3y PFS) and three year's
recurrence free survival(3y RFS) are the major endpoints of this study. Every three months
the patients will be evaluated with necessary modalities such as physical examination, blood
test, radiography, computed tomography, magnetic resonance and/or positron emission
topography until three year after the last radiotherapy/chemotherapy.
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