Metastatic Malignant Neoplasm to Brain Clinical Trial
Official title:
Neurocognitive Outcome of Conformal Whole Brain Radiotherapy With or Without Hippocampal Avoidance for Brain Metastases: A Phase II Single Blind Randomized Trial
Brain metastases are the most common brain tumors in adults. It is estimated that around
10-30% of cancer patients would develop brain metastases during the course of their illness.
Whole brain radiotherapy (WBRT) is the treatment of choice for the majority of patients with
brain metastases. WBRT yields high radiologic response rate (27~56%) and is effective in
rapid palliation of neurologic symptoms as well as prolongs time to neurocognitive function
decline caused by intracranial lesions. By using conventional fractionation, 33% of patients
developed late neurocognitive toxicity while memory impairment was the most common symptom.
The incidence is even higher when a formal and sensitive neurocognitive assessment was
prospectively evaluated. With more long-term survivors nowadays, it has become increasingly
important to minimize neurocognitive function decline and maintain quality of life in
patients with brain metastasis.
The function of hippocampus is cooperation in learning, consolidation and retrieval of
information and essential for formation of new memories. Bilateral and unilateral radiation
injury of the hippocampus is known to alter learning and memory formation. Several
preclinical studies support the hypothesis of hippocampus-mediated cognitive dysfunction by
ionizing radiation. Clinical studies show increase in radiation dose to hippocampus is
associated with subsequent neurocognitive function impairment in adult and pediatric
patients. Furthermore, the preliminary result of Radiation Therapy Oncology Group (RTOG) 0933
suggested hippocampal avoidance significant reduce the mean relative decline at 4 months from
30% in historical cohort with WBRT to 7% in experimental cohort.
Previous studies showed brain structures other than hippocampus are also associated with
radiation-induced decline in neurocognitive function. There is presence of placebo effect for
interventions seeking improvement in neurocognitive function. In present study, a single
blind randomized phase II trial is designed to investigate the effectiveness of
neurocognitive function preservation using conformal WBRT with or without hippocampal
avoidance.
This is a single institutional, randomized phase II study to assess the neurocognitive
outcome of conformal WBRT with or without hippocampal avoidance in patients with multiple
brain metastases.
Patients will be randomly assigned 1:1 to receive conformal WBRT with or without hippocampal
avoidance using permuted blocks within strata that are defined by Graded Prognostic
Assessment (GPA) score and baseline neurocognitive status. All patients and co-investigators
except the principal investigator and attending radiation oncologists will be blinded for
treatment groups.
The whole brain planning target volume (PTV) will receive 30 Gy in 10 fractions. Treatment
will be delivered once daily, 5 fractions per week, over 2 to 2.5 weeks. Breaks in treatment
should be minimized.
Hippocampal Avoidance WBRT:
The dose is prescribed such as 90% of cranial content PTV is covered by the prescription
dose.
Maximum dose to 2% of the PTV (D2%) is 37.5 Gy, and minimum dose to 98% of the PTV (D98%) is
25 Gy. Minimum dose to 100% of the hippocampal avoidance regions is 10 Gy, and dose to any
point within the hippocampal avoidance regions cannot exceed 17 Gy.
Conformal WBRT:
The dose is prescribed such as 95% of cranial content PTV is covered by the prescription
dose.
Maximum dose to 1% of the PTV (D1%) is 36 Gy, and minimum dose to 99% of the PTV (D99%) is 27
Gy.
Follow-up & Assessment
Side effect evaluation:
- Acute (≤ 90 days from WBRT start) toxicities (CTCAE ver.4)
- Late (> 90 days from WBRT start) toxicities (CTCAE ver.4)
Functional evaluation: at baseline, 2-, 4- ,and 6-month, every 3 months for 12 months until
intracranial disease progression or death after WBRT
- Neurocognitive function
- Self-reported cognitive functioning (two items from EORTC Quality of Life
Questionnaire-C30 Taiwan)
- Health-related quality of life specific for brain neoplasms (EORTC Quality of Life
Questionnaire-Brain Neoplasm Taiwan)
Efficacy evaluation:
- Follow-up brain MRI at 4-, 9- ,and 12-month until intracranial disease progression, or
death.
- Overall survival
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