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Radiation Doses and Fractionation Schedules in Non-low Risk Ductal Carcinoma In Situ (DCIS) of the Breast

T

Trans Tasman Radiation Oncology Group

Status

Active, not recruiting

Conditions

Carcinoma, Ductal, Breast

Treatments

Radiation: Standard WB fractionation
Radiation: Standard WB fractionation+Boost
Radiation: Shorter WB fractionation
Radiation: Shorter WB fractionation + Boost

Study type

Interventional

Funder types

Other
NETWORK

Identifiers

NCT00470236
BOOG 2009-03 (Other Identifier)
BIG 3-07 (Other Identifier)
IBCSG 38-10 (Other Identifier)
NCIC CTG MA.33 (Other Identifier)
TROG 07.01
EORTC 22085-10083 (Other Identifier)
SCTBG 2009MayPR55 (Other Identifier)
ICORG 10-06 (Other Identifier)
NHMRC 454390 (Other Grant/Funding Number)

Details and patient eligibility

About

Hypotheses:

  1. The addition of tumour bed boost after BCS in women with non-low risk DCIS reduces the risk of local recurrence (invasive or intraductal recurrence in the ipsilateral breast).
  2. The risk of local recurrence in the shorter fractionation arm is not worse than that for the standard fractionation arm.
  3. A molecular signature predictive of invasive recurrence of DCIS will be detectable and the molecular signature may eventually have clinical utility for therapy individualization.

Overall Objectives:

  1. To improve the outcome of women with non-low risk DCIS treated with breast conserving therapy.
  2. To individualize treatment selection for women with DCIS to achieve long term disease control with minimal toxicity.

Full description

Specific objectives:

  1. To evaluate time to local recurrence in women with DCIS treated with breast conserving surgery followed by:

    • whole breast RT alone versus whole breast RT plus tumour bed boost;
    • RT using the standard fractionation schedule versus the shorter schedule.

  2. To evaluate time to disease recurrence and overall survival in women with DCIS treated with breast conserving surgery followed by:

    • whole breast RT alone versus whole breast RT plus tumour bed boost;
    • RT using the standard fractionation schedule versus the shorter schedule.

  3. To compare the toxicity of:

    • whole breast RT alone versus whole breast RT plus tumour bed boost;
    • RT using the standard fractionation schedule versus the shorter schedule.

  4. To compare the cosmetic outcome of:

    • whole breast RT alone versus whole breast RT plus tumour bed boost;
    • RT using the standard fractionation schedule versus the shorter schedule.

  5. To identify a molecular signature predictive of invasive recurrence of DCIS to facilitate therapy individualization.

  6. To assess inter-relationship of biomarkers and relationship between biomarker expression and specific histopathologic features of DCIS.

  7. To evaluate the quality of life of women treated with:

    • whole breast RT alone versus whole breast RT plus tumour bed boost;
    • RT using the standard fractionation schedule versus the shorter schedule.
Read more

Enrollment

1,608 patients

Sex

Female

Ages

18+ years old

Volunteers

No Healthy Volunteers

Inclusion criteria

Patients must fulfill all of the following criteria for admission to study:

  • Women ≥ 18 years.

  • Histologically proven DCIS of the breast without an invasive component.

  • Bilateral mammograms performed within 6 months prior to randomization.

  • Clinically node-negative.

  • Treated by breast conserving surgery (primary excision or re-excision) with complete microscopic excision and clear radial margins of ≥1 mm* (*Patients with superficial or deep resection margin of <1 mm are eligible if surgery has removed all of the intervening breast tissue from the subcutaneous tissue to the pectoralis fascia).

  • Women who are at high risk of local recurrence due to:

    • Age < 50 years; OR

    • Age ≥ 50 years plus at least one of the following:

      • Symptomatic presentation
      • Palpable tumour
      • Multifocal disease
      • Microscopic tumour size ≥ 1.5 cm in maximum dimension
      • Intermediate or high nuclear grade
      • Central necrosis
      • Comedo histology
      • Radial* surgical resection margin < 10 mm. (*Patients with superficial or deep resection margin of < 10 mm are eligible if surgery has not removed all of the intervening breast tissue from the subcutaneous tissue to the pectoralis fascia.)

  • Assessed by surgeon and radiation oncologist to be suitable for breast conserving therapy including whole breast RT.

  • Ability to tolerate protocol treatment.

  • Protocol RT should preferably commence within 8 weeks but must commence no later than 12 weeks from the last surgical procedure.

  • ECOG performance status 0, 1 or 2.

  • Patient's life expectancy > 5 years.

  • Availability for long-term follow-up.

  • Written informed consent.

Exclusion criteria

Patients who fulfill any of the following criteria are not eligible for admission to study:

  • Multicentric disease or extensive microcalcifications that could not be completely excised by breast conserving surgery with radial margins of ≥1 mm*.

    *Patients with superficial and/or deep margin of <1 mm are eligible if surgery has removed all of the intervening breast tissue from the subcutaneous tissue to the pectoralis fascia.

  • Presence of tumour cells in lymph nodes detected using H&E or immunohistochemical examination (if lymph node biopsy or dissection has been performed).

  • Locally recurrent breast cancer.

  • Previous DCIS or invasive cancer of the contralateral breast.

    • Bilateral DCIS of the breasts
    • Synchronous invasive carcinoma of the contralateral breast

  • Other concurrent or previous malignancies except:

    • Non-melanomatous skin cancer;
    • Carcinoma in situ of the cervix or endometrium; and
    • Invasive carcinoma of the cervix, endometrium, colon, thyroid and melanoma treated at least five years prior to study admission without disease recurrence.

  • Serious non-malignant disease that precludes definitive surgical or radiation treatment (e.g., scleroderma, systemic lupus erythematosus, cardiovascular/pulmonary/renal disease).

  • ECOG performance status ≥ 3.

  • Women who are pregnant or lactating.

Trial design

Primary purpose

Treatment

Allocation

Randomized

Interventional model

Parallel Assignment

Masking

None (Open label)

1,608 participants in 4 patient groups

Arm 1 (Standard WB Fractionation)
Active Comparator group
Description:
Whole Breast RT alone - Standard fractionation schedule (50GY/25 Fractions/35days)
Treatment:
Radiation: Standard WB fractionation
Arm 2 (Shorter WB Fractionation)
Experimental group
Description:
Whole Breast RT alone - Shorter fractionation schedule (42.5 Gy/16 fractions/22 days)
Treatment:
Radiation: Shorter WB fractionation
Arm 3 (Standard WB fractionation+Boost)
Active Comparator group
Description:
Whole Breast RT + tumor bed boost - Standard fractionation schedule (50 Gy/25 fractions/35 days; Boost 16 Gy/8 fractions/10 days)
Treatment:
Radiation: Standard WB fractionation+Boost
Arm 4 (Shorter WB fractionation + Boost)
Experimental group
Description:
Whole breast RT + tumour bed boost - Shorter fractionation schedule (42.5 Gy/16 fractions/22 days; Boost 16 Gy/8 fractions/10 days)
Treatment:
Radiation: Shorter WB fractionation + Boost

Trial contacts and locations

120

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Data sourced from clinicaltrials.gov

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