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Clinical Trial Summary

Patients with locally advanced rectal and esophageal carcinomas typically undergo neoadjuvant chemoradiation therapy prior to surgical resection. While response rates to this treatment differ among these three cancers, generally 20-25% of patients exhibit minimal or no response to preoperative chemoradiation therapy while 20-30% exhibit a complete pathologic response, and the remainder receiving a partial response.

This will be a multi-center study of patients with newly diagnosed rectal adenocarcinoma, or anal squamous cell carcinoma (SCC) who will undergo neoadjuvant chemoradiation prior to surgery. The tumor from these patients will be tested to determine whether response to neoadjuvant chemoradiation can be accurately predicted.


Clinical Trial Description

Patients with locally advanced rectal and esophageal carcinomas typically undergo neoadjuvant chemoradiation therapy prior to surgical resection, although the specific chemoradiation regimens may vary. While response rates differ among these three cancers, generally 20-25% of patients exhibit minimal or no response to preoperative chemoradiation therapy while 20-30% exhibit a complete pathologic response, and the remainder receiving a partial response.

In esophageal adenocarcinoma, patients who achieve a complete response tend to have a significantly longer overall survival than those who do not achieve a complete response. Similar data exists for rectal cancer that the degree of responsiveness to chemoradiation regimens dictates survival outcome in patients.

If patients with distinct response profiles can be identified before treatment starts, personalized regimens can be delivered to maximize the benefit in each patient population: complete responders may be spared post-treatment surgical resection, while non responders may consider avoiding ineffective chemoradiation prior to surgery.

Target Population:

Subjects with newly diagnosed rectal adenocarcinoma, or anal squamous cell carcinoma (SCC) who will undergo neoadjuvant chemoradiation prior to surgery.

350 patient samples will be included in this validation study, given the predicted 25% population size that exhibit pathologic complete response (pathCR) to pre-operative chemo/radiation therapy, and the predicted 25% population size that have no response (exCTRT) to pre-operative treatment.

Study Design:

This will be a multi-center prospective study of up to 350 patients, each having both pre-treatment (prior to chemoradiation) unstained sections on charged slides from the FFPE block that was used for diagnosis of rectal or anal cancer and sections of unstained, post-surgical, resected tissue (pathologic confirmation of treatment response based upon endoscopy or ultrasound can be accepted in place of post-surgical resected tissue). Per the CLIA-compliant SOPs (Appendix A), one slide will be stained with H&E to define the area of tumor within the tissue, and the remaining slides will be used for immunohistochemical (IHC) detection of the biomarkers described above to assess the performance of the proprietary IHC assay. Any remaining slides not used for IHC staining will be used for a parallel gene expression discovery effort using TaqMan high throughput RT-PCR analysis (Appendix B, Sub-study 1).

The proprietary assay will be performed under CLIA certified standard operating procedures. The individual assay results, treatment effect, actual survival data, and other clinical data will be analyzed. Initial labeling index data will be used to develop a training set and unique algorithmic approach specifically applicable to rectal and anal carcinoma. The remaining samples will be embargoed for use as an independent test set.

Associated clinical data will be collected :

1. Age of patient at diagnosis

2. Gender

3. Date of diagnosis rectal/anal cancer

4. Histotype of rectal/anal cancer

5. Stage of rectal/anal cancer at diagnosis and again after neoadjuvant treatment (if available)

6. Details of imaging performed

7. Clinical and histopathalogical features of primary tumor

8. Details of any genetic testing performed.

9. Extent/approach of surgical resection

10. Date of last contact

11. First progression documentation (Y/N). If yes, location of first progression and date of first progression.

12. Method of diagnosis of first progression.

13. Death documentation (Y/N). If yes, date of death, cause of death.

14. Pre-operative treatments received:

1. Start/stop date of radiation

2. Radiation dose, fractions given, interruptions to treatment (Y/N), reasons if Yes

3. Start/stop date of chemotherapy

4. Chemotherapeutic agent(s) and doses, interruptions to treatment (Y/N), reasons if Yes

15. Post-surgical treatments received:

1. Start/stop date of radiation

2. Radiation dose, fractions given, interruptions to treatment (Y/N), reasons if Yes

3. Start/stop date of chemotherapy

4. Chemotherapeutic agent(s) and doses, interruptions to treatment (Y/N), reasons if Yes ;


Study Design


Related Conditions & MeSH terms


NCT number NCT02407561
Study type Observational
Source Castle Biosciences Incorporated
Contact
Status Terminated
Phase N/A
Start date February 2015
Completion date July 2016

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