1. Radiation Oncology Trials Alone & in Multimodality Settings Stephen M. Hahn
University of Pennsylvania School of Medicine
Philadelphia, PA USA
3. The Evolution of Radiation Therapy Key points to make:
Completely new carriage and leaf design to
Other improvements made:
Reduced Head Diameter by 10 cm from previous “Standard” MLC Key points to make:
Completely new carriage and leaf design to
Other improvements made:
Reduced Head Diameter by 10 cm from previous “Standard” MLC
4. Effect of underdosage and overdosage This means,an increase in tumour dose necessitates a decrease in toxicity in order to increase tumour control. This is expressed as an increase of the therapeutic ratio.This means,an increase in tumour dose necessitates a decrease in toxicity in order to increase tumour control. This is expressed as an increase of the therapeutic ratio.
6. Trials of Radiation Therapy Alone Target Volume
Organs at Risk
Quality Assurance
Dose
Volume
Time
Assessment of Toxicities
8. Interpretation of radiotherapy trials:��Radiotherapy outcomes are dependent upon technical factors ���
10. Quality Control-Radiation Standard dose and fractionation schedules
Specify fields or target volumes – be precise
Specify doses to target volumes
IMRT vs. 3-D conformal radiotherapy
CT-based vs. conventional simulation
Field verification
Dose inhomogeneity
11. Standard slide with 2 logosStandard slide with 2 logos
12. Multi-Modality Radiation Trials
13. Translation to the Clinic -Potential Problems Baseline response rate
Baseline cure rate
Baseline toxicity
Interdependence of one modality on the other for therapeutic effect
Competing risks for end-point of interest
14. Factors Affecting Radiation Sensitivity Intrinsic Factors
Ras mutational status
EGFR
DNA repair capabilities
DNA methylation
Extrinsic Factors
Tumor microenvironment – hypoxia
pH
Tumor vasculature – ‘normalization’
17. Chemoradiotherapy An improved therapeutic index should be the goal
Effect of chemoradiotherapy on the tumor compared to the effect of chemoradiotherapy on normal tissue toxicity
Classically there are 4 ways to define the interaction
spatial cooperation
toxicity independence
radioprotectors
radiation sensitizers
Steel & Peckham IJROBP 5:85, 1979
18. Therapeutic Gain This means,an increase in tumour dose necessitates a decrease in toxicity in order to increase tumour control. This is expressed as an increase of the therapeutic ratio.This means,an increase in tumour dose necessitates a decrease in toxicity in order to increase tumour control. This is expressed as an increase of the therapeutic ratio.
20. Preclinical Studies-Rationale Combining chemotherapy with radiation requires a rationale preferably grounded in supporting preclinical data
There should be convincing preclinical data that indicates that the combination is either
Efficacious (radiation sensitization)
No overlapping toxicities (toxicity independence)
21. Preclinical Studies-Rationale Demonstrate in vitro radiosensitization in human tumor cell lines
Demonstrate in vivo radiosensitization in human tumor models
Demonstrate the lack of sensitization of normal tissues
Preclinical studies should use clinically relevant doses and schedules of agents & XRT
22. Question # 1
23. Question # 2
24. Phase I Studies of Drugs and Radiation
25. Phase I studies-Endpoints The goals of combined modality Phase I studies are similar to single agent studies
However, the design and application often differs
The primary endpoint is usually an assessment of toxicity with the goal of identifying a recommended Phase II dose
26. Phase I studies The definition of the recommended Phase II dose: the doses and schedules of both the drug and radiation when used in combination
It is NOT the same as the maximally tolerated dose although MTD can be used to identify the recommended Phase II dose
The schedule and dose of radiation may be very different from that used with each agent alone
27. Phase I studies Data helpful for the design of the study
Single agent pharmacokinetic data from the relevant scheduling regimen
Continuous dosing during XRT vs. once a week dosing
Single agent pharmacodynamic data
Agent’s affect on a molecular target that is relevant to the interaction between XRT and radiation
Single agent safety data
28. Phase I studies-Design Issues Patient selection
What tumor sites?
The answer to this question impacts greatly upon the assessment of toxicity.
The selection of tumor site may also be impacted by the agent being used in combination with XRT (think C225 and HNC)
Curative or palliative radiotherapy?
This will affect total radiation dose and fractionation
This will affect the patient population and perhaps the ability to tolerate combined modality therapy
In general, Phase I data are generated from studies that are cancer-specific and/or site-specific.
29. Phase I studies-Design Issues What doses and schedules of the agent should be selected?
If the goal is radiosensitization, then delivery of the agent during as many fractions of radiation is desirable
The schedule and dose may also be impacted by the known characteristics and target of the agent
What doses of radiation should be selected?
A typical approach especially in the curative setting is to start with a standard radiation dose; however escalation of the radiation dose may be desirable in certain clinical situations
30. Phase I studies-Design Issues A limited dose-escalation design is typical for these studies
Dose-limiting toxicity rules
Grade IV hematological toxicity
Grade III non-hematological toxicity
Exceptions should be considered – Grade III diarrhea in the setting of upper abdominal XRT
Breaks during XRT
31. Phase I studies-Design Issues Dose escalation rules
Standard Phase I dose escalation rules are acceptable especially if multiple agents are being used (including conventional chemotherapy)
Consider using a toxicity assessment in association with clinical or biological endpoints
Particularly with targeted agents, defining the “optimal biologic dose” might be appropriate
Be careful because the biological endpoint is a surrogate for clinical efficacy and this may not be known during the Phase I development period
32. Phase I studies-Endpoints Toxicity criteria
Consider XRT or combined modality-specific criteria (RTOG)
Toxicity assessment is typically during the entire radiation course and some defined period of time after XRT, e.g. 30 days
How do we assess late effects?
There are practical and time limitations
Bevacizumab and thoracic radiation
33. Phase I studies-Design Issues Think about the next step in development
What is the standard therapy for the tumor site being treated?
What is the role of conventional chemotherapy?
How should surgery (if appropriate) be integrated?
How should chemotherapy be integrated?
34. Anti-Angiogenic Therapy Hypothesis: Can anti-angiogenic therapy augment the effect of radiation therapy and chemotherapy on rectal cancer?
Immature and inefficient blood vessels could be pruned by eliminating excess endothelial cells --> “Normalized Vasculature” --> Improved delivery of nutrients and therapeutics
37. Antiangiogenic therapy: �Conclusions from Preliminary In- vivo Data The addition of antiangiogenic agents to chemoradiation programs:
increases tumor perfusion/reduces hypoxia
increases tumor radioresponse
does not appear to increase (skin) toxicity
increases chemoresponse
38. Phase I Study
39. Rectal Cancer: Phase I Study (Schema) Bevacizumab 5-10 mg/kg, 2 weeks prior to XRT
Level Bev (q2wk) 5-FU (mg/m2/d) RT (Gy)
1 5 mg/kg 225 50.4
2 10 mg/kg 225 50.4
Bevacizumab: 4 Infusions
After determination of MTD, 20 additional pts to be treated
Willett et al. Nature Medicine, 2004
40. Study Endpoints / Correlates MTD of Bevacizumab with EBRT and 5-FU
Preliminary Data: pCR, LC, PFS, S
Correlative studies
Functional imaging (PET, CT perfusion studies)
Interstitial Pressure Measurement
Circulating Endothelial Cells and Precursors
Tissue
Serum and Urine
42. Phase II studies The decision to proceed with a combined modality Phase II study is dependent upon the safety and early efficacy results from the Phase I trial
The primary goals of a Phase II combined modality study is efficacy
43. Phase II trials-Endpoints Response rates are often not helpful for selecting efficacious regimens
Delayed time to response with XRT
Residual unevaluable masses vs. scarring
Progressive disease outside of the XRT field
Underlying high local response rates to XRT
44. Phase II trials-Endpoints Consider other efficacy endpoints
Complete response rate
Pathological complete response rate
Local or locoregional control rates
Time to progression
Survival
The endpoint selected will depend upon the tumor & the current standard therapy
45. Phase II trials-Endpoints Additional toxicity data both acute and late toxicity are essential components
Collection of late toxicity data in the larger group of patients that constitutes a Phase II study will be helpful as the Phase III study is designed
46. Phase II trials-Design Early stopping rules for toxicity (most likely acute toxicity) should be considered
Early stopping rules for low response rates compared to historical controls may also be a useful design consideration
Usually dramatic differences in response must be seen for early stopping rules to be implemented
47. Phase III Study Generally a major interdependence of modalities
Quality control of each modality can be of enormous importance in defining whether a therapy should be used
Produces an interaction which can effect the study outcome
48. Special Considerations in trials that include surgical therapy The surgeon as a prognostic factor
Adherence to surgical technique
Quality control
Experience of the surgeon
The pathologist as a variable
Quality control
49. COMBINED MODALITY THERAPY One must consider multiple issues in study design
Biologic interaction between modalities
Patient selection
Quality control
Base line data- response, toxicity, survival
The same issues as in other studies,but approached differently
