Delayed Sentinel Lymph Node Biopsy in Ductal Cancer in Situ
The trial aims to investigate the use of superparamagnetic iron oxide (SPIO) nanoparticles as a tracer for delayed sentinel lymph node dissection (d-SLND) in patients where upfront axillary surgery (SLND) is oncologically deemed unnecessary and should be avoided. This includes but is not limited to patients with a preoperative diagnosis of ductal cancer in situ of the breast (DCIS), an unclear BIRADS 4-5 planned for diagnostic excision or women planned for risk reducing mastectomy. SPIO is injected in the primary operation, and should final specimen pathology demonstrate invasive breast cancer, only then is an operation in the axilla (d-SLND) performed.
Inclusion Criteria
- Inclusion Criteria: A. Preoperative diagnosis of DCIS, of any grade and any size if planned for mastectomy. B. Planned Risk-reducing mastectomy, if it would be considered for upfront SLND due to institutional practice or in case of an individualised recommendation. C. Any case with a preoperative diagnosis of pre-invasive or unclear lesion, that upfront SLND would be otherwise considered, such as, but not limited to: - Patients with a preoperative diagnosis of DCIS grade 3 any size or, DCIS grade 2 larger than or equal to 20 mm on mammography and planned for breast conserving surgery or - Patients with a preoperative diagnosis of DCIS on core biopsy with a palpable mass on clinical examination or mass effect on radiology or - Patients with a preoperative diagnosis of DCIS with suspicion of micro-invasion on core biopsy or - Patients with a mammographic/ultrasound/MRI finding, suspicious for breast cancer (BIRADS 4 or 5) planned for diagnostic excision with breast conserving surgery, with no definitive diagnosis of invasive cancer or - Patients with a preoperative diagnosis of DCIS, any grade, any size and planned for a complex oncoplastic procedure or - Patients with a preoperative diagnosis of DCIS, any grade, any size and planned for a procedure that may compromise detection rate for a future SLND, such as, but not confined to: lesions in the upper outer quadrant or the axillary tail, removal of the nipple areola complex and so on or - The above mentioned categories with a preoperative diagnosis of pleomorphic Lobular Cancer in Situ (pLCIS), classic Lobular Neoplasia (LN) or Atypical Ductal Hyperplasia (ADH). Exclusion Criteria: - Intolerance/hypersensitivity to iron, dextran compounds or SPIO - An iron overload disease - Patient deprived of liberty or under guardianship - Pregnant or lactating patients
Additional locations may be listed on ClinicalTrials.gov for NCT04722692.
Locations matching your search criteria
United States
Texas
Houston
The SentiNot 2.0 protocol aims to elucidate the effectivity and accuracy of the delayed
sentinel lymph node dissection concept (dSLND) when upfront SLND is considered
unnecessary, such as in the setting of a preoperative diagnosis of DCIS, in cases of
unclear BIRADS 4 or 5 lesions that are planned for diagnostic excisional biopsy or in
selected cases of risk reducing mastectomy. Acknowledging the large variance of practice
in this setting, the study aims to address pragmatism to allow for inclusion. For this
reason, the trial is designed separately and independently for mastectomy and breast
conserving surgery, so that participating sites can recruit as fitting in their practice.
In patients included in the SentiNot 2.0 trial, SPIO (MagTrace,2.0 ml) is injected up to
24 hours preoperatively or perioperatively during primary breast surgery on patients with
a preoperative diagnosis of DCIS (or suspicious lesions with no clear diagnosis of
invasive cancer but, considered for SLND). The SPIO is injected close to the lesion. If
injected less than 24 hours before the operation, a 5 minute massage should be performed.
Planned breast surgery is performed. The transcutaneous magnetic counts by SentiMag in
the axilla is measured at the end of the breast procedure, so as to allow for
confirmation that SLND may be identified. Thus,the SLN is consequently marked with SPIO,
but not excised.
In this manner, women that have pure DCIS on final histopathological examination have
avoided unnecessary upfront SLND.
If there is underlying invasive breast cancer on final histopathological examination,
SLND will be performed at a second operation (d-SLND). A preoperative injection of
radioisotope (RI) RI will be added to maximize the chance to detect the SLN. SLND will
start with a registration of the magnetic and isotope signal in the axilla, and the
incision will be placed in relation to the signal. In patients that have undergone
mastectomy, tracers are to be injected intracutaneously in the lateral part of the
mastectomy scar. The routine use of blue dye (BD) is strongly advised, but is not
compulsory. However, if no transcutaneous signal for SPIO and RI is measured in the
axilla pre-incision, an injection of BD according local routines will be administered.
Subsequently, SLND will be performed. Patients with upgrade to invasive cancer will
undergo SLND, but will be randomized with an allocation ratio of 1:1 to SentiMag first or
Radioactive probe first. This will mandate the "principal modality" to perform SLND.
Every step of the procedure will be controlled; if the principal modality fails, then the
surgeon will use the "secondary". If the principal modality succeeds, the secondary will
be registered and documented.
The procedure will be divided to the following steps:
- Transcutaneous axillary signal detection
- Subcutaneous axillary detection, after the incision has been performed.
- In situ SLN identification.
- SLN retrieval ex vivo.
- Residual axillary signal ("Background counts"). If a SLND is successfully completed
with the primary modality and no residual axillary signal is detected, before
completing the procedure, the secondary modality will be undertaken to allow for the
detection of "discordance".
Principle modalities maybe either RI or SPIO. If BD is used, dyed lymphatics should be
ignored until failure with both modalities has been reached. The success of each
modality, principal and secondary, will be controlled per step. If the surgeon documents
principle modality failure for a given step, this is to be documented. The
intention-to-treat principle will apply, but if there is failure of the modality
randomized as principle, then the per-protocol-analysis principle will apply. All SLNs
(magnetic, brown, radioactive, blue) will be removed. Palpable nodes may be removed
according to surgeon discretion, but should be reported as such. Total technique failure
has to be discussed with the patient in advance, and a plan with patient consent
consisting of no-surgery, sampling, axillary dissection or treatment according to
intraoperative decision has to be available. If no SLN is found, the procedure performed
(axillary clearance, sampling. etc) should be discussed in advance with the patient. The
SLN may be sent for frozen section in order to avoid a third operation, if SLN metastases
are present.
Standard of care patients (SLND performed upfront for diagnoses included in the inclusion
criteria or patients going to l-SLND without SPIO) may also be enrolled in the study
prospectively as a control arm.Additionally, patient preference will be tolerated and
results will be reported for study secondary and other pre-specified endpoints. Patients
in the control group has to be informed that their un-identified data will be used as a
comparison and, an oral consent has to be given before surgery regardless whether SLND is
planned or not. This will allow for controlled real world data from a prospective control
arm in fashion of a cohort.
Trial PhasePhase III
Trial Typetreatment
Lead OrganizationUppsala University Hospital
- Primary IDUUBreast01
- Secondary IDsNCI-2022-02319
- ClinicalTrials.gov IDNCT04722692