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MANAGEMENT OF EARLY BREAST 
CANCER 
Dr. Akhil Kapoor 
Department of Radiation Oncology 
Acharya Tulsi Regional Cancer Treatment & 
Research Institute, Bikaner 
Acharya Tulsi Regional Cancer Center, Bikaner
STAGING 
Acharya Tulsi Regional Cancer Center, 
Bikaner
Acharya Tulsi Regional Cancer Center, 
Bikaner
Acharya Tulsi Regional Cancer Center, 
Bikaner
PATHOLOGIC N STAGE 
 pN1mi = Micrometastasis ≤ 2mm size 
(0.2-2mm) 
or, <200 cells 
Acharya Tulsi Regional Cancer Center, 
Bikaner
STAGES INCLUDED IN EARLY BREAST CANCER 
Acharya Tulsi Regional Cancer Center, 
Bikaner
LCIS 
 Multicentric in 90% of specimens 
 Bilateral in 35-59% cases 
 10% Invasive ca has associated LCIS. 
Must at diagnosis: 
 Bilateral Mammogram 
 Pathology Review 
Importance of Mammogram: 
 LCIS: A marker for increased risk for subsequent 
development of invasive (usually ductal carcinoma) 
Acharya Tulsi Regional Cancer Center, 
Bikaner
 Surgical Excision Biopsy is must to proceed for 
management. 
 Management is done according to associated DCIS 
or Invasive Ca disregarding the presence of LCIS. 
 If margins are positive for LCIS, additional surgery 
to obtain clear margins for LCIS is not required. 
Acharya Tulsi Regional Cancer Center, 
Bikaner
LCIS AS SOLE HISTOLOGIC DX 
 Most widely accepted approach: Close observation 
with mammographic surveillance 
 Patients with highest risk (Young; diffuse high grade 
lesion; Family history): 
Bilateral Prophylactic Mastectomy 
 Tamoxifen alone reduces the risk by 56%. 
Acharya Tulsi Regional Cancer Center, 
Bikaner
PAGET’S DISEASE 
 Rare entity: <5% of all Breast Ca cases; In fifth-sixth 
decade. 
 D/d: Eczema (B/L in Eczema) 
 Palpable mass present in 50% cases (Invasive Ca 
in 90%). 
 If no palpable mass, 66-86% underlying DCIS. 
 Prognosis and management according to 
underlying disease. 
Acharya Tulsi Regional Cancer Center, 
Bikaner
USUAL MANAGEMENT: 
 Complete excision of Nipple Areola Complex with 
microscopically clear margins for both Paget’s and 
associated malignancy. 
Followed by: 
 Whole Breast RT 
 5 Year Local Recurrence Rate of 5.2% (EORTC 
Study) 
Acharya Tulsi Regional Cancer Center, 
Bikaner
DCIS 
 Pure DCIS: No indication of Axillary dissection. 
 Apparent pure DCIS: Upto 25% cases turn out to 
be Invasive Ca in lumpectomy specimen. 
 Thus, if Mastectomy is performed: SLNB preferred. 
 If lumpectomy includes Axillary tail, SLNB preferred 
(as surgery compromises future SLNB in the rare 
event of associated Invasive Ca) 
Acharya Tulsi Regional Cancer Center, 
Bikaner
RECURRENCE 
 Recurrence is 50% DCIS and 50% Invasive Ca. 
 Risk Factors for Recurrence: 
1) Age <50yrs 
2) Palpable mass 
3) Close (<1mm) or involved margins 
4) High Grade 
5) Diameter >1cm 
6) Presence of Comedo Necrosis. 
Acharya Tulsi Regional Cancer Center, 
Bikaner
VAN NUYS INDEX 
more 
 Modified VNPI includes AGE as well. 
Acharya Tulsi Regional Cancer Center, 
Bikaner
 Whole Breast RT following lumpectomy reduces the 
recurrence rate by 50% in DCIS. 
 Boost to tumor bed by 10 Gy is recommended in 
cases with close margins and age <50yrs. 
 MRI may be advised in patients suspected to have 
multi centric disease. 
Acharya Tulsi Regional Cancer Center, 
Bikaner
 Patients without any high risk feature: Surgical 
Excision alone is sufficient. 
 Tamoxifen addition for 5 years (NSABP B-24 trial): 
 Reduces the recurrence rate by 3.4% (HR 0.30, 
p<0.001) in ipsilateral IBTR. 
 Absolute reduction in Contra lateral Breast Ca by 
3.2% (HR 0.68, p=0.02). 
Thus, Tamoxifen is added in ER+ DCIS after 
Lumpectomy and Radiation. 
Acharya Tulsi Regional Cancer Center, 
Bikaner
 Her 2 status in pure DCIS: No significance. 
Indications of Simple Mastectomy in DCIS: 
 Multicentric Disease 
 Diffuse Microcalcifications 
 Family History 
Acharya Tulsi Regional Cancer Center, 
Bikaner
Acharya Tulsi Regional Cancer Center, 
Bikaner
WORK UP FOR EARLY BREAST CA 
Hematological Tests 
 Baseline CBC, RFT, LFT 
(as Surgery and Chemotherapy are to be given) 
 Serum Alkaline phosphatase: Raised in patients 
with Bone Mets 
"bone burns, liver lasts" : Heat Unstable ALP in Bone 
diseases. 
Acharya Tulsi Regional Cancer Center, 
Bikaner
PATHOLOGY 
 Pathology Review 
 Determination of ER, PR and Her-2-neu Status 
Acharya Tulsi Regional Cancer Center, 
Bikaner
IMAGING STUDIES 
o Bilateral Mammogram ± USG 
o Bone Scan: 
Indicated in 
 Localised bone pain 
 Elevated ALP 
o Chest CT: If pulmonary symptoms 
o Baseline Echo/ MUGA Scan (MultiGated 
Acquistion- Tc99m) 
Acharya Tulsi Regional Cancer Center, 
Bikaner
ABDOMINAL ± PELVIC CT: 
Indications: 
 Abnormal Physical Examination of abdomen or 
pelvis 
 Abdominal Symptoms 
 Abnormal LFT 
 Raised ALP 
Acharya Tulsi Regional Cancer Center, 
Bikaner
BREAST MRI 
Requirements: 
 Expert Breast Imaging Team 
 Dedicated Breast Coils 
 Facility for MRI guided Needle Sampling or wire 
localisation of MRI detected abnormalities. 
Indications: 
 To evaluate dense breasts (young) 
 Breast Ca in Pregnancy 
 In patients with Positive Axilla with Occult primary (not 
identified with Mammogram). 
 To determine Multicentric Disease in I/L Breast 
 Screening of C/L Breast in high risk patients 
Acharya Tulsi Regional Cancer Center, 
Bikaner
PET-CT 
 Not usually indicated. 
 Indicated in situations when standard imaging is 
equivocal/suspicious especially in locally 
advanced/metastatic breast cancer. 
Acharya Tulsi Regional Cancer Center, 
Bikaner
FOR T3N1MO 
Usually Part of the Initial Work up: 
 Chest CT 
 Abdominal CT 
 Bone Scan 
Acharya Tulsi Regional Cancer Center, 
Bikaner
BCS 
Acharya Tulsi Regional Cancer Center, 
Bikaner 
(in absence of Extensive Intraductal Component-Boost Required)
PRE OPERATIVE SYSTEMIC THERAPY 
 Indicated if patient desires BCS and fulfills the 
criteria for BCS except for size. 
 Core Biopsy with placement of image-detectable 
marker to demarcate the tumor bed for post-CT 
surgical management. 
 Clinically negative axilla should be checked by 
USG, suspicious nodes should be sampled by 
FNAC or core needle and clipped with image 
detectable marker. 
Acharya Tulsi Regional Cancer Center, 
Bikaner
 Similarly, clinically positive nodes must be sampled 
and clipped. 
 Clipped Nodes that are positive on histology must 
be removed at the time of Surgery. 
Acharya Tulsi Regional Cancer Center, 
Bikaner
 CT regimes are similar in neo-adjuvant and 
adjuvant settings. 
 Endocrine therapy alone may be considered in 
Post-menopausal patients with receptor positive 
disease (Aromatase inhibitor). 
 Her-2 + disease treated with systemic therapy 
along with at least 9 weeks of trastuzumab. 
Acharya Tulsi Regional Cancer Center, 
Bikaner
DEFINITION OF MENOPAUSE 
 PM Range: FSH >25 IU/l; E2 <200pmol/l 
Acharya Tulsi Regional Cancer Center, 
Bikaner
HER 2 NEGATIVE 
Acharya Tulsi Regional Cancer Center, 
Bikaner
HER 2 NEGATIVE 
Acharya Tulsi Regional Cancer Center, 
Bikaner
Acharya Tulsi Regional Cancer Center, 
Bikaner
HER 2 POSITIVE 
Acharya Tulsi Regional Cancer Center, 
Bikaner
Acharya Tulsi Regional Cancer Center, 
Bikaner
MOA PERTUZUMAB 
 PERJETA targets a different domain on the HER2 
receptor than trastuzumab, allowing the 
combination to provide a more comprehensive 
blockade of HER2-driven signaling pathways. 
Acharya Tulsi Regional Cancer Center, 
Bikaner
PERTUZUMAB 
 The pCR rates were 39.3% in patients who 
received pertuzumab plus trastuzumab and 
docetaxel 
 and 21.5 % in patients who received trastuzumab 
plus docetaxel. 
 (adjusted p-value = 0.0063). 
 The pCR rates and magnitude of improvement with 
the addition of pertuzumab were lower in the 
subgroup of patients with hormone receptor-positive 
tumors compared to patients with hormone 
receptor-negative tumors. 
Acharya Tulsi Regional Cancer Center, 
Bikaner
PREOP SYSTEMIC THERAPY 
 Confirmed Progressive disease anytime: 
Proceed to MRM 
 If CR/PR with possible BCS: 
Proceed to Lumpectomy 
Acharya Tulsi Regional Cancer Center, 
Bikaner
BASELINE DOCUMENTATION OF “TARGET” AND 
“NON-TARGET” LESIONS 
 All measurable lesions up to a maximum of five lesions per 
organ and 10 lesions in total, representative of all involved 
organs should be identified as target lesions and recorded 
and measured at baseline. 
 Target lesions should be selected on the basis of their size 
(lesions with the longest diameter) and their suitability for 
accurate repeated measurements (either by imaging 
techniques or clinically). 
Acharya Tulsi Regional Cancer Center, 
Bikaner
 A sum of the longest diameter (LD) for all target 
lesions will be calculated and reported as the 
baseline sum LD. The baseline sum LD will be used 
as reference by which to characterize the objective 
tumor response. 
 All other lesions should be identified as non-target 
lesions and should also be recorded at baseline. 
Measurements of these lesions are not required, 
but the presence or absence of each should be 
noted throughout follow-up. 
Acharya Tulsi Regional Cancer Center, 
Bikaner
EVALUATION OF TARGET LESIONS 
 Complete Response (CR): Disappearance of all target 
lesions 
 Partial Response (PR): At least a 30% decrease in the 
sum of the LD of target lesions, taking as reference the 
baseline sum LD 
 Stable Disease (SD): Neither sufficient shrinkage to 
qualify for PR nor sufficient increase to qualify for PD, 
taking as reference the smallest sum LD since the 
treatment started 
 Progressive Disease (PD): At least a 20% increase in 
the sum of the LD of target lesions, taking as reference 
the smallest sum LD recorded since the treatment 
started or the appearance of one or more new lesions 
Acharya Tulsi Regional Cancer Center, 
Bikaner
EVALUATION OF NON-TARGET LESIONS 
 Complete Response (CR): Disappearance of all 
non-target lesions and normalization of tumor 
marker level 
 Incomplete Response/ Stable Disease (SD): 
Persistence of one or more non-target lesion(s) 
or/and maintenance of tumor marker level above 
the normal limits 
 Progressive Disease (PD): Appearance of one or 
more new lesions and/or unequivocal progression 
of existing non-target lesions 
Acharya Tulsi Regional Cancer Center, 
Bikaner
BCS WITH SURGICAL AXILLARY STAGING 
 No Axillary Node: RT to Whole Breast ± Boost 
APBI in selected patients 
 +ve Axillary Node: RT to whole breast ± Boost 
+ Nodal RT ± IMN RT 
Acharya Tulsi Regional Cancer Center, 
Bikaner
Acharya Tulsi Regional Cancer Center, 
Bikaner
TUMOR BED BOOST 
 Rationale: 65%-80% of breast recurrences after 
BCS + RT occur around the primary tumor site. 
 Clark et al. noted in 1,504 patients a greater 
incidence of failures at 10 years of 17% in those to 
whom no boost was delivered, compared with 11% 
in those who received doses of 5 to 15 Gy at the 
primary excision site (P = .03) 
Acharya Tulsi Regional Cancer Center, 
Bikaner
Currently, most institutions prefer electron beam 
boost because 
 of its relative ease in setup, 
 outpatient setting, 
 lower cost, 
 decreased time demands on the physician, 
 and excellent results compared with 192Ir implants. 
Acharya Tulsi Regional Cancer Center, 
Bikaner
EORTC TRIAL 
 Bartelink et al. after BCS and axillary dissection, 
stage I or II, received 50 Gy of radiation to the 
whole breast in 2-Gy fractions over a 5-week period 
 Randomly assigned to receive either no further 
local treatment (2,657 patients) or a boost of 16 Gy, 
usually given in 8 fractions by electron beam (2,661 
patients). 
 The 5-year actuarial rates of local recurrence were 
7.3% and 4.3%, respectively (P <.001). 
Acharya Tulsi Regional Cancer Center, 
Bikaner
INTERNATIONAL BREAST CANCER STUDY 
GROUP TRIALS 
 Premenopausal with 1-3+LN: LRR 19-27% if 
G2-3 disease with vascular invasion 
but that risk was <15% if they had G1 disease with 
no vascular invasion. 
 Postmenopausal with 1-3+LN: 
G3 disease and T>2 cm LRR 24% 
as compared with <15% for those with G1–2 
disease with T<2 cm. 
Acharya Tulsi Regional Cancer Center, 
Bikaner
DOSE OF RADIATION 
 Dose of 45-50Gy at 1.8-2Gy per fraction given 5 
fractions per week. 
 Another dose schedule: 42.5 Gy at 2.66Gy per 
fraction in 16 fractions 
 Boost to tumor bed in patients at high risk (Age<50 
years, high grade disease) with 10-16Gy at 2 Gy 
per fraction. 
 Dose to regional nodes: 50-50.4Gy at 1.8-2Gy per 
fraction (±Scar Boost to 60Gy at 2Gy per fraction). 
Acharya Tulsi Regional Cancer Center, 
Bikaner
HYPOFRACTIONATION IN BREAST 
Acharya Tulsi Regional Cancer Center, 
Bikaner
START TRIAL A 
 Criteria: Early breast cancer (pT1-3, pN0-1 M0); 
BCS or Mastectomy 
 50 Gy in 25 fractions over 5 weeks 
 41.6 Gy/3.2Gy per fraction in 13 fractions over 5 
weeks, or 
 39 Gy/3Gy per fraction in 13 fractions over 5 weeks 
 The overall treatment time was kept constant in all 
three arms 
 Allowed treatment of regional lymph nodes 
(supraclavicular and axillary), used in 20%. 
Acharya Tulsi Regional Cancer Center, 
Bikaner
RESULTS 
 Median follow-up was 9·3 years. 
 10-year rates of local-regional relapse: 
 50 Gy: 7.4% 
 41.6 Gy: 6.3% (p=0.65) 
 39 Gy: 8.8% (p=0.41) 
Acharya Tulsi Regional Cancer Center, 
Bikaner
START TRIAL B 
 Criteria: Early breast cancer (pT1-3, pN0-1 M0) 
 50 Gy/2 Gy per fraction, 25 fractions over 5 wks, 
 40 Gy/2.67 Gy per fraction,15 fractions over 3 wks. 
 Results: 
 10-year rates of local-regional relapse: 
 50 Gy: 5.5% 
 40 Gy: 4.3% (p=0.21) 
Acharya Tulsi Regional Cancer Center, 
Bikaner
COSMESIS 
Acharya Tulsi Regional Cancer Center, 
Bikaner
COSMESIS 
 Breast induration, telangiectasia, and breast 
oedema were significantly less common normal 
tissue effects in the Hypofractionated group than in 
the 50 Gy group. 
Acharya Tulsi Regional Cancer Center, 
Bikaner
DFS IN START A & B 
Acharya Tulsi Regional Cancer Center, 
Bikaner
SUBGROUP ANALYSIS 
Acharya Tulsi Regional Cancer Center, 
Bikaner
 Inclusion Criteria: 
Invasive Breast Ca, BCS, Margins clear, N0 
 Control group: 50.0 Gy in 25 fractions over a period 
of 35 days 
 Hypofractionated group: 42.5 Gy in 16 fractions 
over a period of 22 days. 
Acharya Tulsi Regional Cancer Center, 
Bikaner
 No Nodal radiation; No Boost 
RESULTS 
The risk of local recurrence at 10 years: 
 6.7% standard irradiation 
 6.2% hypofractionated regimen 
Good or excellent cosmetic outcome at 10 years: 
 71.3% in control group 
 69.8% in hypofractionated 
Acharya Tulsi Regional Cancer Center, 
Bikaner
Acharya Tulsi Regional Cancer Center, 
Bikaner
HAZARD RATIO FOR SUBGROUPS 
Acharya Tulsi Regional Cancer Center, 
Bikaner
SELECTION CRITERIA FOR APBI (ASTRO) 
 Age>60 yrs 
 pT1N0, ER + 
 Margins Negative by at least 2mm 
 BRCA 1, 2 Negative 
 LVSI Absent 
 DCIS Absent 
 Ext Intraductal Component Absent 
 Unicentric 
 Unifocal (same quadrant) 
 Histology: IDC/Mucinous/Tubular/Colloid 
 No previous NACT 
 Asso. LCIS allowed 
Acharya Tulsi Regional Cancer Center, 
Bikaner
DOSE IN APBI 
 34Gy/3.4Gy per fraction/2 fractions per day 6 hrs 
apart for 5 days 
 For APBI by EBRT, 
38.5Gy/3.85Gy per fraction/2 fractions per day 6 hrs 
apart for 5 days 
Acharya Tulsi Regional Cancer Center, 
Bikaner
FOLLOWING TOTAL MASTECTOMY
 The finding comes from a meta-analysis of 
individual data for a total of 8135 women 
participating in clinical trials who were followed for 
an average of 11 years; 1314 of these women 
were found to have 1 to 3 positive nodes. 
Acharya Tulsi Regional Cancer Center, 
Bikaner
EBCTCG STUDY 
 In women who had 1-3+ nodes, PMRT reduced the 
RR by 32% and reduced the breast cancer mortality 
rate by 20%. 
 The benefit was similar whether women had only 
1+ node or whether they had 2 or 3+ nodes. 
 For women with ≥4 + nodes (n = 1772), RT reduced 
overall recurrence by 21% and breast cancer 
mortality by 13%. 
Acharya Tulsi Regional Cancer Center, 
Bikaner
 Woodward et al. found that the risk of LRR after 
mastectomy and anthracycline-based 
chemotherapy was only 13% for patients with stage 
II disease and one to three positive lymph nodes. 
 However, at the same institution, patients with 
similarly staged disease treated with PMRT had a 
LRR risk of only 3%. 
Acharya Tulsi Regional Cancer Center, 
Bikaner
COFACTORS FOR >15% LRR AFTER 
MASTECTOMY + CT WITH 1-3 +LN 
Acharya Tulsi Regional Cancer Center, 
Bikaner
CLINICAL CASE 
 A 40 year lady with lump in upper outer quadrant of 
breast underwent MRM with final HPR as follows: 
pT1N0 (T=0.4 cm), Metaplastic histology, ER+, PR-, 
Her 2+; other parameters favorable. 
Acharya Tulsi Regional Cancer Center, 
Bikaner
QUESTION 
 What next in management? 
Ans: Adjuvant endocrine therapy is sufficient. 
Acharya Tulsi Regional Cancer Center, 
Bikaner
DECISION CHART 
Acharya Tulsi Regional Cancer Center, 
Bikaner
QUESTION 
 What if the same patient was ER, PR Negative? 
Ans: No adjuvant therapy 
Acharya Tulsi Regional Cancer Center, 
Bikaner
DECISION TREE
CLINICAL CASE 
 A 40 year lady with lump in upper outer quadrant of 
breast underwent MRM with final HPR as follows: 
pT1N0 (T=1 cm), Ductal histology, ER+, PR-, Her 2- 
; other parameters favorable. 
Ques: Next Management? 
Acharya Tulsi Regional Cancer Center, 
Bikaner
ONCOTYPE DX 
 Analyzes a panel of 21 genes within a tumor 
to determine a Recurrence Score. 
 The RS is a number between 0 and 100 that 
corresponds to a specific likelihood of 
breast cancer recurrence within 10 years of 
the initial diagnosis. 
Acharya Tulsi Regional Cancer Center, 
Bikaner
GENES ANALYZED IN ONCOTYPE DX 
Acharya Tulsi Regional Cancer Center, 
Bikaner
USE 
Oncotype DX demonstrated both 
 Prognostic significance (the capability of predicting 
distant recurrence) 
 Predictive significance (the capability of the test to 
assess the potential benefit of additional adjuvant 
chemotherapy). 
Acharya Tulsi Regional Cancer Center, 
Bikaner
Acharya Tulsi Regional Cancer Center, 
Bikaner
Kaplan-Meier plots for distant recurrence comparing treatment with tamoxifen (Tam) alone 
versus treatment with tamoxifen plus chemotherapy (Tam + chemo). 
Paik S et al. JCO 2006;24:3726-3734 
©2006 by American Society of Clinical Oncology 
Acharya Tulsi Regional Cancer Center, 
Bikaner
Relative and absolute risks of chemotherapy (chemo) benefit as a function of recurrence 
score (RS) risk category. 
Paik S et al. JCO 2006;24:3726-3734 
©2006 by American Society of Clinical Oncology 
Acharya Tulsi Regional Cancer Center, 
Bikaner
Acharya Tulsi Regional Cancer Center, 
Bikaner
CLINICAL CASE 
 A 40 year lady with lump in upper outer quadrant of 
breast underwent MRM with final HPR as follows: 
pT1N0 (T=0.8 cm), Mucinous histology, ER+, PR-, 
other parameters favorable. 
Next Management? 
Ans: No adjuvant therapy 
Acharya Tulsi Regional Cancer Center, 
Bikaner
DECISION TREE
FOLLOW UP 
Acharya Tulsi Regional Cancer Center, 
Bikaner
Acharya Tulsi Regional Cancer Center, 
Bikaner
THANKS 
Acharya Tulsi Regional Cancer Center, 
Bikaner
NEXT PRESENTATION 
Management of Locally Advanced 
Breast Cancer 
Dr. Satya Narayan 
Acharya Tulsi Regional Cancer Center, 
Bikaner

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Management of Early Breast Cancer (by Dr. Akhil Kapoor)

  • 1. MANAGEMENT OF EARLY BREAST CANCER Dr. Akhil Kapoor Department of Radiation Oncology Acharya Tulsi Regional Cancer Treatment & Research Institute, Bikaner Acharya Tulsi Regional Cancer Center, Bikaner
  • 2. STAGING Acharya Tulsi Regional Cancer Center, Bikaner
  • 3. Acharya Tulsi Regional Cancer Center, Bikaner
  • 4. Acharya Tulsi Regional Cancer Center, Bikaner
  • 5. PATHOLOGIC N STAGE  pN1mi = Micrometastasis ≤ 2mm size (0.2-2mm) or, <200 cells Acharya Tulsi Regional Cancer Center, Bikaner
  • 6. STAGES INCLUDED IN EARLY BREAST CANCER Acharya Tulsi Regional Cancer Center, Bikaner
  • 7. LCIS  Multicentric in 90% of specimens  Bilateral in 35-59% cases  10% Invasive ca has associated LCIS. Must at diagnosis:  Bilateral Mammogram  Pathology Review Importance of Mammogram:  LCIS: A marker for increased risk for subsequent development of invasive (usually ductal carcinoma) Acharya Tulsi Regional Cancer Center, Bikaner
  • 8.  Surgical Excision Biopsy is must to proceed for management.  Management is done according to associated DCIS or Invasive Ca disregarding the presence of LCIS.  If margins are positive for LCIS, additional surgery to obtain clear margins for LCIS is not required. Acharya Tulsi Regional Cancer Center, Bikaner
  • 9. LCIS AS SOLE HISTOLOGIC DX  Most widely accepted approach: Close observation with mammographic surveillance  Patients with highest risk (Young; diffuse high grade lesion; Family history): Bilateral Prophylactic Mastectomy  Tamoxifen alone reduces the risk by 56%. Acharya Tulsi Regional Cancer Center, Bikaner
  • 10. PAGET’S DISEASE  Rare entity: <5% of all Breast Ca cases; In fifth-sixth decade.  D/d: Eczema (B/L in Eczema)  Palpable mass present in 50% cases (Invasive Ca in 90%).  If no palpable mass, 66-86% underlying DCIS.  Prognosis and management according to underlying disease. Acharya Tulsi Regional Cancer Center, Bikaner
  • 11. USUAL MANAGEMENT:  Complete excision of Nipple Areola Complex with microscopically clear margins for both Paget’s and associated malignancy. Followed by:  Whole Breast RT  5 Year Local Recurrence Rate of 5.2% (EORTC Study) Acharya Tulsi Regional Cancer Center, Bikaner
  • 12. DCIS  Pure DCIS: No indication of Axillary dissection.  Apparent pure DCIS: Upto 25% cases turn out to be Invasive Ca in lumpectomy specimen.  Thus, if Mastectomy is performed: SLNB preferred.  If lumpectomy includes Axillary tail, SLNB preferred (as surgery compromises future SLNB in the rare event of associated Invasive Ca) Acharya Tulsi Regional Cancer Center, Bikaner
  • 13. RECURRENCE  Recurrence is 50% DCIS and 50% Invasive Ca.  Risk Factors for Recurrence: 1) Age <50yrs 2) Palpable mass 3) Close (<1mm) or involved margins 4) High Grade 5) Diameter >1cm 6) Presence of Comedo Necrosis. Acharya Tulsi Regional Cancer Center, Bikaner
  • 14. VAN NUYS INDEX more  Modified VNPI includes AGE as well. Acharya Tulsi Regional Cancer Center, Bikaner
  • 15.  Whole Breast RT following lumpectomy reduces the recurrence rate by 50% in DCIS.  Boost to tumor bed by 10 Gy is recommended in cases with close margins and age <50yrs.  MRI may be advised in patients suspected to have multi centric disease. Acharya Tulsi Regional Cancer Center, Bikaner
  • 16.  Patients without any high risk feature: Surgical Excision alone is sufficient.  Tamoxifen addition for 5 years (NSABP B-24 trial):  Reduces the recurrence rate by 3.4% (HR 0.30, p<0.001) in ipsilateral IBTR.  Absolute reduction in Contra lateral Breast Ca by 3.2% (HR 0.68, p=0.02). Thus, Tamoxifen is added in ER+ DCIS after Lumpectomy and Radiation. Acharya Tulsi Regional Cancer Center, Bikaner
  • 17.  Her 2 status in pure DCIS: No significance. Indications of Simple Mastectomy in DCIS:  Multicentric Disease  Diffuse Microcalcifications  Family History Acharya Tulsi Regional Cancer Center, Bikaner
  • 18. Acharya Tulsi Regional Cancer Center, Bikaner
  • 19. WORK UP FOR EARLY BREAST CA Hematological Tests  Baseline CBC, RFT, LFT (as Surgery and Chemotherapy are to be given)  Serum Alkaline phosphatase: Raised in patients with Bone Mets "bone burns, liver lasts" : Heat Unstable ALP in Bone diseases. Acharya Tulsi Regional Cancer Center, Bikaner
  • 20. PATHOLOGY  Pathology Review  Determination of ER, PR and Her-2-neu Status Acharya Tulsi Regional Cancer Center, Bikaner
  • 21. IMAGING STUDIES o Bilateral Mammogram ± USG o Bone Scan: Indicated in  Localised bone pain  Elevated ALP o Chest CT: If pulmonary symptoms o Baseline Echo/ MUGA Scan (MultiGated Acquistion- Tc99m) Acharya Tulsi Regional Cancer Center, Bikaner
  • 22. ABDOMINAL ± PELVIC CT: Indications:  Abnormal Physical Examination of abdomen or pelvis  Abdominal Symptoms  Abnormal LFT  Raised ALP Acharya Tulsi Regional Cancer Center, Bikaner
  • 23. BREAST MRI Requirements:  Expert Breast Imaging Team  Dedicated Breast Coils  Facility for MRI guided Needle Sampling or wire localisation of MRI detected abnormalities. Indications:  To evaluate dense breasts (young)  Breast Ca in Pregnancy  In patients with Positive Axilla with Occult primary (not identified with Mammogram).  To determine Multicentric Disease in I/L Breast  Screening of C/L Breast in high risk patients Acharya Tulsi Regional Cancer Center, Bikaner
  • 24. PET-CT  Not usually indicated.  Indicated in situations when standard imaging is equivocal/suspicious especially in locally advanced/metastatic breast cancer. Acharya Tulsi Regional Cancer Center, Bikaner
  • 25. FOR T3N1MO Usually Part of the Initial Work up:  Chest CT  Abdominal CT  Bone Scan Acharya Tulsi Regional Cancer Center, Bikaner
  • 26. BCS Acharya Tulsi Regional Cancer Center, Bikaner (in absence of Extensive Intraductal Component-Boost Required)
  • 27. PRE OPERATIVE SYSTEMIC THERAPY  Indicated if patient desires BCS and fulfills the criteria for BCS except for size.  Core Biopsy with placement of image-detectable marker to demarcate the tumor bed for post-CT surgical management.  Clinically negative axilla should be checked by USG, suspicious nodes should be sampled by FNAC or core needle and clipped with image detectable marker. Acharya Tulsi Regional Cancer Center, Bikaner
  • 28.  Similarly, clinically positive nodes must be sampled and clipped.  Clipped Nodes that are positive on histology must be removed at the time of Surgery. Acharya Tulsi Regional Cancer Center, Bikaner
  • 29.  CT regimes are similar in neo-adjuvant and adjuvant settings.  Endocrine therapy alone may be considered in Post-menopausal patients with receptor positive disease (Aromatase inhibitor).  Her-2 + disease treated with systemic therapy along with at least 9 weeks of trastuzumab. Acharya Tulsi Regional Cancer Center, Bikaner
  • 30. DEFINITION OF MENOPAUSE  PM Range: FSH >25 IU/l; E2 <200pmol/l Acharya Tulsi Regional Cancer Center, Bikaner
  • 31. HER 2 NEGATIVE Acharya Tulsi Regional Cancer Center, Bikaner
  • 32. HER 2 NEGATIVE Acharya Tulsi Regional Cancer Center, Bikaner
  • 33. Acharya Tulsi Regional Cancer Center, Bikaner
  • 34. HER 2 POSITIVE Acharya Tulsi Regional Cancer Center, Bikaner
  • 35. Acharya Tulsi Regional Cancer Center, Bikaner
  • 36. MOA PERTUZUMAB  PERJETA targets a different domain on the HER2 receptor than trastuzumab, allowing the combination to provide a more comprehensive blockade of HER2-driven signaling pathways. Acharya Tulsi Regional Cancer Center, Bikaner
  • 37. PERTUZUMAB  The pCR rates were 39.3% in patients who received pertuzumab plus trastuzumab and docetaxel  and 21.5 % in patients who received trastuzumab plus docetaxel.  (adjusted p-value = 0.0063).  The pCR rates and magnitude of improvement with the addition of pertuzumab were lower in the subgroup of patients with hormone receptor-positive tumors compared to patients with hormone receptor-negative tumors. Acharya Tulsi Regional Cancer Center, Bikaner
  • 38. PREOP SYSTEMIC THERAPY  Confirmed Progressive disease anytime: Proceed to MRM  If CR/PR with possible BCS: Proceed to Lumpectomy Acharya Tulsi Regional Cancer Center, Bikaner
  • 39. BASELINE DOCUMENTATION OF “TARGET” AND “NON-TARGET” LESIONS  All measurable lesions up to a maximum of five lesions per organ and 10 lesions in total, representative of all involved organs should be identified as target lesions and recorded and measured at baseline.  Target lesions should be selected on the basis of their size (lesions with the longest diameter) and their suitability for accurate repeated measurements (either by imaging techniques or clinically). Acharya Tulsi Regional Cancer Center, Bikaner
  • 40.  A sum of the longest diameter (LD) for all target lesions will be calculated and reported as the baseline sum LD. The baseline sum LD will be used as reference by which to characterize the objective tumor response.  All other lesions should be identified as non-target lesions and should also be recorded at baseline. Measurements of these lesions are not required, but the presence or absence of each should be noted throughout follow-up. Acharya Tulsi Regional Cancer Center, Bikaner
  • 41. EVALUATION OF TARGET LESIONS  Complete Response (CR): Disappearance of all target lesions  Partial Response (PR): At least a 30% decrease in the sum of the LD of target lesions, taking as reference the baseline sum LD  Stable Disease (SD): Neither sufficient shrinkage to qualify for PR nor sufficient increase to qualify for PD, taking as reference the smallest sum LD since the treatment started  Progressive Disease (PD): At least a 20% increase in the sum of the LD of target lesions, taking as reference the smallest sum LD recorded since the treatment started or the appearance of one or more new lesions Acharya Tulsi Regional Cancer Center, Bikaner
  • 42. EVALUATION OF NON-TARGET LESIONS  Complete Response (CR): Disappearance of all non-target lesions and normalization of tumor marker level  Incomplete Response/ Stable Disease (SD): Persistence of one or more non-target lesion(s) or/and maintenance of tumor marker level above the normal limits  Progressive Disease (PD): Appearance of one or more new lesions and/or unequivocal progression of existing non-target lesions Acharya Tulsi Regional Cancer Center, Bikaner
  • 43. BCS WITH SURGICAL AXILLARY STAGING  No Axillary Node: RT to Whole Breast ± Boost APBI in selected patients  +ve Axillary Node: RT to whole breast ± Boost + Nodal RT ± IMN RT Acharya Tulsi Regional Cancer Center, Bikaner
  • 44. Acharya Tulsi Regional Cancer Center, Bikaner
  • 45. TUMOR BED BOOST  Rationale: 65%-80% of breast recurrences after BCS + RT occur around the primary tumor site.  Clark et al. noted in 1,504 patients a greater incidence of failures at 10 years of 17% in those to whom no boost was delivered, compared with 11% in those who received doses of 5 to 15 Gy at the primary excision site (P = .03) Acharya Tulsi Regional Cancer Center, Bikaner
  • 46. Currently, most institutions prefer electron beam boost because  of its relative ease in setup,  outpatient setting,  lower cost,  decreased time demands on the physician,  and excellent results compared with 192Ir implants. Acharya Tulsi Regional Cancer Center, Bikaner
  • 47. EORTC TRIAL  Bartelink et al. after BCS and axillary dissection, stage I or II, received 50 Gy of radiation to the whole breast in 2-Gy fractions over a 5-week period  Randomly assigned to receive either no further local treatment (2,657 patients) or a boost of 16 Gy, usually given in 8 fractions by electron beam (2,661 patients).  The 5-year actuarial rates of local recurrence were 7.3% and 4.3%, respectively (P <.001). Acharya Tulsi Regional Cancer Center, Bikaner
  • 48. INTERNATIONAL BREAST CANCER STUDY GROUP TRIALS  Premenopausal with 1-3+LN: LRR 19-27% if G2-3 disease with vascular invasion but that risk was <15% if they had G1 disease with no vascular invasion.  Postmenopausal with 1-3+LN: G3 disease and T>2 cm LRR 24% as compared with <15% for those with G1–2 disease with T<2 cm. Acharya Tulsi Regional Cancer Center, Bikaner
  • 49. DOSE OF RADIATION  Dose of 45-50Gy at 1.8-2Gy per fraction given 5 fractions per week.  Another dose schedule: 42.5 Gy at 2.66Gy per fraction in 16 fractions  Boost to tumor bed in patients at high risk (Age<50 years, high grade disease) with 10-16Gy at 2 Gy per fraction.  Dose to regional nodes: 50-50.4Gy at 1.8-2Gy per fraction (±Scar Boost to 60Gy at 2Gy per fraction). Acharya Tulsi Regional Cancer Center, Bikaner
  • 50. HYPOFRACTIONATION IN BREAST Acharya Tulsi Regional Cancer Center, Bikaner
  • 51. START TRIAL A  Criteria: Early breast cancer (pT1-3, pN0-1 M0); BCS or Mastectomy  50 Gy in 25 fractions over 5 weeks  41.6 Gy/3.2Gy per fraction in 13 fractions over 5 weeks, or  39 Gy/3Gy per fraction in 13 fractions over 5 weeks  The overall treatment time was kept constant in all three arms  Allowed treatment of regional lymph nodes (supraclavicular and axillary), used in 20%. Acharya Tulsi Regional Cancer Center, Bikaner
  • 52. RESULTS  Median follow-up was 9·3 years.  10-year rates of local-regional relapse:  50 Gy: 7.4%  41.6 Gy: 6.3% (p=0.65)  39 Gy: 8.8% (p=0.41) Acharya Tulsi Regional Cancer Center, Bikaner
  • 53. START TRIAL B  Criteria: Early breast cancer (pT1-3, pN0-1 M0)  50 Gy/2 Gy per fraction, 25 fractions over 5 wks,  40 Gy/2.67 Gy per fraction,15 fractions over 3 wks.  Results:  10-year rates of local-regional relapse:  50 Gy: 5.5%  40 Gy: 4.3% (p=0.21) Acharya Tulsi Regional Cancer Center, Bikaner
  • 54. COSMESIS Acharya Tulsi Regional Cancer Center, Bikaner
  • 55. COSMESIS  Breast induration, telangiectasia, and breast oedema were significantly less common normal tissue effects in the Hypofractionated group than in the 50 Gy group. Acharya Tulsi Regional Cancer Center, Bikaner
  • 56. DFS IN START A & B Acharya Tulsi Regional Cancer Center, Bikaner
  • 57. SUBGROUP ANALYSIS Acharya Tulsi Regional Cancer Center, Bikaner
  • 58.  Inclusion Criteria: Invasive Breast Ca, BCS, Margins clear, N0  Control group: 50.0 Gy in 25 fractions over a period of 35 days  Hypofractionated group: 42.5 Gy in 16 fractions over a period of 22 days. Acharya Tulsi Regional Cancer Center, Bikaner
  • 59.  No Nodal radiation; No Boost RESULTS The risk of local recurrence at 10 years:  6.7% standard irradiation  6.2% hypofractionated regimen Good or excellent cosmetic outcome at 10 years:  71.3% in control group  69.8% in hypofractionated Acharya Tulsi Regional Cancer Center, Bikaner
  • 60. Acharya Tulsi Regional Cancer Center, Bikaner
  • 61. HAZARD RATIO FOR SUBGROUPS Acharya Tulsi Regional Cancer Center, Bikaner
  • 62. SELECTION CRITERIA FOR APBI (ASTRO)  Age>60 yrs  pT1N0, ER +  Margins Negative by at least 2mm  BRCA 1, 2 Negative  LVSI Absent  DCIS Absent  Ext Intraductal Component Absent  Unicentric  Unifocal (same quadrant)  Histology: IDC/Mucinous/Tubular/Colloid  No previous NACT  Asso. LCIS allowed Acharya Tulsi Regional Cancer Center, Bikaner
  • 63. DOSE IN APBI  34Gy/3.4Gy per fraction/2 fractions per day 6 hrs apart for 5 days  For APBI by EBRT, 38.5Gy/3.85Gy per fraction/2 fractions per day 6 hrs apart for 5 days Acharya Tulsi Regional Cancer Center, Bikaner
  • 65.  The finding comes from a meta-analysis of individual data for a total of 8135 women participating in clinical trials who were followed for an average of 11 years; 1314 of these women were found to have 1 to 3 positive nodes. Acharya Tulsi Regional Cancer Center, Bikaner
  • 66. EBCTCG STUDY  In women who had 1-3+ nodes, PMRT reduced the RR by 32% and reduced the breast cancer mortality rate by 20%.  The benefit was similar whether women had only 1+ node or whether they had 2 or 3+ nodes.  For women with ≥4 + nodes (n = 1772), RT reduced overall recurrence by 21% and breast cancer mortality by 13%. Acharya Tulsi Regional Cancer Center, Bikaner
  • 67.  Woodward et al. found that the risk of LRR after mastectomy and anthracycline-based chemotherapy was only 13% for patients with stage II disease and one to three positive lymph nodes.  However, at the same institution, patients with similarly staged disease treated with PMRT had a LRR risk of only 3%. Acharya Tulsi Regional Cancer Center, Bikaner
  • 68. COFACTORS FOR >15% LRR AFTER MASTECTOMY + CT WITH 1-3 +LN Acharya Tulsi Regional Cancer Center, Bikaner
  • 69. CLINICAL CASE  A 40 year lady with lump in upper outer quadrant of breast underwent MRM with final HPR as follows: pT1N0 (T=0.4 cm), Metaplastic histology, ER+, PR-, Her 2+; other parameters favorable. Acharya Tulsi Regional Cancer Center, Bikaner
  • 70. QUESTION  What next in management? Ans: Adjuvant endocrine therapy is sufficient. Acharya Tulsi Regional Cancer Center, Bikaner
  • 71. DECISION CHART Acharya Tulsi Regional Cancer Center, Bikaner
  • 72. QUESTION  What if the same patient was ER, PR Negative? Ans: No adjuvant therapy Acharya Tulsi Regional Cancer Center, Bikaner
  • 74. CLINICAL CASE  A 40 year lady with lump in upper outer quadrant of breast underwent MRM with final HPR as follows: pT1N0 (T=1 cm), Ductal histology, ER+, PR-, Her 2- ; other parameters favorable. Ques: Next Management? Acharya Tulsi Regional Cancer Center, Bikaner
  • 75.
  • 76. ONCOTYPE DX  Analyzes a panel of 21 genes within a tumor to determine a Recurrence Score.  The RS is a number between 0 and 100 that corresponds to a specific likelihood of breast cancer recurrence within 10 years of the initial diagnosis. Acharya Tulsi Regional Cancer Center, Bikaner
  • 77. GENES ANALYZED IN ONCOTYPE DX Acharya Tulsi Regional Cancer Center, Bikaner
  • 78. USE Oncotype DX demonstrated both  Prognostic significance (the capability of predicting distant recurrence)  Predictive significance (the capability of the test to assess the potential benefit of additional adjuvant chemotherapy). Acharya Tulsi Regional Cancer Center, Bikaner
  • 79. Acharya Tulsi Regional Cancer Center, Bikaner
  • 80. Kaplan-Meier plots for distant recurrence comparing treatment with tamoxifen (Tam) alone versus treatment with tamoxifen plus chemotherapy (Tam + chemo). Paik S et al. JCO 2006;24:3726-3734 ©2006 by American Society of Clinical Oncology Acharya Tulsi Regional Cancer Center, Bikaner
  • 81. Relative and absolute risks of chemotherapy (chemo) benefit as a function of recurrence score (RS) risk category. Paik S et al. JCO 2006;24:3726-3734 ©2006 by American Society of Clinical Oncology Acharya Tulsi Regional Cancer Center, Bikaner
  • 82. Acharya Tulsi Regional Cancer Center, Bikaner
  • 83. CLINICAL CASE  A 40 year lady with lump in upper outer quadrant of breast underwent MRM with final HPR as follows: pT1N0 (T=0.8 cm), Mucinous histology, ER+, PR-, other parameters favorable. Next Management? Ans: No adjuvant therapy Acharya Tulsi Regional Cancer Center, Bikaner
  • 85. FOLLOW UP Acharya Tulsi Regional Cancer Center, Bikaner
  • 86. Acharya Tulsi Regional Cancer Center, Bikaner
  • 87. THANKS Acharya Tulsi Regional Cancer Center, Bikaner
  • 88. NEXT PRESENTATION Management of Locally Advanced Breast Cancer Dr. Satya Narayan Acharya Tulsi Regional Cancer Center, Bikaner

Editor's Notes

  1. Kaplan-Meier plots for distant recurrence comparing treatment with tamoxifen (Tam) alone versus treatment with tamoxifen plus chemotherapy (Tam + chemo). (A) All patients; (B) low risk (recurrence score [RS] < 18); (C) intermediate risk (RS 18-30); (D) high risk (RS ≥ 31). The number of patients at risk and the number of distant recurrences (in parentheses) are provided below each part of the figure.
  2. Relative and absolute risks of chemotherapy (chemo) benefit as a function of recurrence score (RS) risk category. Int, intermediate; DRF, distant recurrence free.