Non-invasive breast carcinoma
Non-invasive breast carcinoma is a type of breast cancer and a common entity... since the introduction of radiologic breast screening.
Viewed simplistically, it can neatly be divided into the discussion of two entities:
- Ductal carcinoma in situ (DCIS).
- Lobular carcinoma in situ (LCIS).
Invasive breast cancer is dealt with in the article invasive breast cancer.
Ductal neoplasia
Overview
This category includes:
- Atypical ductal hyperplasia (ADH).
- Ductal carcinoma in situ (DCIS).
The difference between ADH and DCIS is:
- The degree of nuclear atypia; high grade is DCIS.
- The extent; small lesions are ADH, large lesions (low-grade) DCIS.
Is it ductal neoplasia?
FEHUT versus ADH versus DCIS
- Breast duct lumen with too many cells; this is common problem is breast pathology.[1]
- The general DDx for this scenario is: EHUT versus ADH versus DCIS.
Notes:
- EHUT = epithelial hyperplasia of the usual type, AKA florid epithelial hyperplasia of the usual type (FEHUT).
- ADH = atypical ductal hyperplasia.
- DCIS = ductal carcinoma in situ.
Tabular comparison - histomorphology
Comparison of EHUT, ADH and DCIS (memory device: CLEAN = cell uniformity, luminal spaces, extent/size, arch., nuclei):
EHUT | ADH | DCIS | |
Cellular composition | varied | focal uniformity | uniform |
Lumina | slits/irregular spaces; cells haphazardly arranged around lumen |
irregular spaces, no slits | circular "punched-out"; cells side-by-side + equally spaced @ interface |
Extent | usually lobulocentric | limited extent | extensive |
Architecture | irregular/swirling | DCIS-like | DCIS architecture (solid, cribriform, papillary, micropapillary) |
Nuclei (intranuclear spacing) |
variable | hyperchromatic & uniform |
evenly spaced |
Treatment - implications:
- EHUT - nothing; EHUT is benign.
- ADH - simple excision, i.e. lumpectomy.
- DCIS - excision (lumpectomy) + radiation.
- Invasive ductal carcinoma - excision with sentinel lymph node biopsy (for staging)[2] and radiation.
- Positive sentinel node - systemic chemotherapy. (???)
IHC
Usual ductal hyperplasia (AKA FEHUT) vs. ADH/DCIS:[3][4]
- FEHUT: ER-low/CK5-high profile.
- ADH/DCIS: ER-high/CK5-low.
Where:
- ER-high = diffuse strong staining in >90% of cells.
- CK5-high = mosaic pattern of staining in >20% of cells
- CK5-low = absent or staining in <20% of cells.
Atypical ductal hyperplasia
- Abbreviated ADH.
General
- Molecular studies have shown it is the same thing as low-grade DCIS; thus, some have called for abolition of the term.[5]
- ADH is considered an indication for a lumpectomy.[6]
Epidemiology:
- Relative risk of breast cancer, based on a median follow-up of 8 years, in a case control study of US registered nurses, is 3.7.[9]
Microscopic
Features:
- Cytologic and architectural featurs same as low-grade DCIS.
- Limited extent - either:[10]
- < Two complete ducts.
- < 2 mm.
Images:
Ductal carcinoma in situ
- Abbreviated DCIS.
General
- Diagnosis based on nuclear abnormalities and architecture.
- It is typically picked-up during radiologic screening.
Microscopic
Features:
- Architectural changes:
- Equal spacing of cells - "cookie cutter" look.
- Cells line-up along lumen/glandular spaces - form "Roman briges".
- Architecture suggestive of DCIS - see Subtypes of DCIS.
- Nuclear changes:
- Nuclear enlargement - at least 2-3x size of RBC - key feature.
- Compared to RBCs to grade DCIS - see Grading DCIS.
- Compare sizes of nuclei if you cannot find RBCs.
- Compared to RBCs to grade DCIS - see Grading DCIS.
- Nuclear pleomorphism - important feature.
- Nuclear enlargement - at least 2-3x size of RBC - key feature.
- +/-Mitoses.
Note:
- Apocrine changes of cytoplasm -- nuclei should be ~4x RBC for low grade, 5x RBC for high grade.[11]
Subtypes of DCIS
Subtypes are based on architecture:
- Solid.
- No spaces between cells.
- Cribriform.
- Honeycomb-like appearance: circular holes.
- "Cookie cutter" appearance/"punched-out" appearance/"Roman bridges" -- cells surround the circular holes.
- Papillary.
- Papillae with fibrovascular cores.
- Micropapillary.
- Small papillae without fibrovascular cores.
- Have "drum stick" shape.
NOTE: comedonecrosis - used to be considered a separate subtype -- essentially solid type DCIS with necrosis.
Grading DCIS
Graded 1-3 (low-high)[12] - compare lesional nuclei to one another.
- Grade 1:
- Nuclei 2-3x size of RBC.
- No necrosis.
- Grade 2:
- Nuclei 2-3x size of RBC.
- +/-Necrosis.
- Grade 3:
- Nuclei >3x size of RBC.
- Necrosis usually present.
Notes:
- It is often hard to find RBCs when you want 'em. DCIS is pleomorphic.
- If no RBCs are present to compare with compare the nuclei to one another.
- If you see nuclei >3x larger than their neigbour you're ready to call DCIS Grade 3.
Size criteria for low-grade DCIS
ADH is diagnosed if the lesion is small - specifically:[13][14]
- < Two membrane-bound spaces.
- < 2 mm extent.
The treatment is similar; ADH and DCIS are both excised.
The differences are:
- DCIS is cancer, i.e. this has life insurance implications.
- Radiation treatment - DCIS is irradiated; ADH does not get radiation.
Micrometastasis in DCIS
Micrometastasis in DCIS - not significant.[15][16]
Lobular neoplasia
Overview
Includes:
- Atypical lobular hyperplasia (ALH).
- Lobular carcinoma in situ (LCIS).
- These entities (ALH, LCIS) are near identical from a histomorphologic perspective.
- The difference is extent of involvement:
- ALH <50% of terminal duct lobular unit (TDLU) is involved.
- LCIS >=50% of TDLU is involved.
Atypical lobular hyperplasia
- Abbreviated ALH.
Microscopic
See LCIS.
Lobular carcinoma in situ
- Abbreviated LCIS.
General
- Management is currently some matter of debate.
- Not detected radiologically - it is an incidental pathologic finding.
Microscopic
- Cells distend the duct.
- Dyscohesive - distinct cell border visible.
- Clear cytoplasm (focally); may have signet ring cell-like appearance.
- Eccentrically placed round nucleus,
- Usually minimal atypia, relatively small ~1-2x size lymphocyte.
- +/-Nucleolus.
Memory device ABCDE:
- Atypia minimal.
- Borders of cells distinct.
- Clear cytoplasm.
- Distend duct.
- Eccentric nucleus.
Subclassification[18]
- Non-PLCIS.
- Type A.
- Nucleus 1-1.5x lymphocyte.
- No nucleolus.
- Type B.
- Nucleus ~2x lymphocyte.
- Nucleolus present.
- Type A.
- PLCIS (pleomorphic lobular carcinoma in situ).
Main DDx:
- Low-grade DCIS.
See also
References
- ↑ O'Malley, Frances P.; Pinder, Sarah E. (2006). Breast Pathology: A Volume in Foundations in Diagnostic Pathology series (1st ed.). Churchill Livingstone. pp. 167-8. ISBN 978-0443066801.
- ↑ Sentinel Lymph Node Biopsy: What Breast Cancer Patients Need to Know. cancernews.com. URL: http://www.cancernews.com/data/Article/202.asp. Accessed on: 9 October 2009.
- ↑ Rabban, JT.; Koerner, FC.; Lerwill, MF. (Jul 2006). "Solid papillary ductal carcinoma in situ versus usual ductal hyperplasia in the breast: a potentially difficult distinction resolved by cytokeratin 5/6.". Hum Pathol 37 (7): 787-93. doi:10.1016/j.humpath.2006.02.016. PMID 16784976.
- ↑ Grin, A.; O'Malley, FP.; Mulligan, AM. (Nov 2009). "Cytokeratin 5 and estrogen receptor immunohistochemistry as a useful adjunct in identifying atypical papillary lesions on breast needle core biopsy.". Am J Surg Pathol 33 (11): 1615-23. doi:10.1097/PAS.0b013e3181aec446. PMID 19675450.
- ↑ Ghofrani, M.; Tapia, B.; Tavassoli, FA. (Dec 2006). "Discrepancies in the diagnosis of intraductal proliferative lesions of the breast and its management implications: results of a multinational survey.". Virchows Arch 449 (6): 609-16. doi:10.1007/s00428-006-0245-y. PMID 17058097.
- ↑ Liberman L, Cohen MA, Dershaw DD, Abramson AF, Hann LE, Rosen PP (May 1995). "Atypical ductal hyperplasia diagnosed at stereotaxic core biopsy of breast lesions: an indication for surgical biopsy". AJR Am J Roentgenol 164 (5): 1111–3. PMID 7717215. http://www.ajronline.org/cgi/pmidlookup?view=long&pmid=7717215.
- ↑ Deshaies, I.; Provencher, L.; Jacob, S.; Côté, G.; Robert, J.; Desbiens, C.; Poirier, B.; Hogue, JC. et al. (Feb 2011). "Factors associated with upgrading to malignancy at surgery of atypical ductal hyperplasia diagnosed on core biopsy.". Breast 20 (1): 50-5. doi:10.1016/j.breast.2010.06.004. PMID 20619647.
- ↑ Margenthaler, JA.; Duke, D.; Monsees, BS.; Barton, PT.; Clark, C.; Dietz, JR. (Oct 2006). "Correlation between core biopsy and excisional biopsy in breast high-risk lesions.". Am J Surg 192 (4): 534-7. doi:10.1016/j.amjsurg.2006.06.003. PMID 16978969.
- ↑ London, SJ.; Connolly, JL.; Schnitt, SJ.; Colditz, GA. (Feb 1992). "A prospective study of benign breast disease and the risk of breast cancer.". JAMA 267 (7): 941-4. PMID 1734106.
- ↑ Tadrous, Paul.J. Diagnostic Criteria Handbook in Histopathology: A Surgical Pathology Vade Mecum (1st ed.). Wiley. pp. 258. ISBN 978-0470519035.
- ↑ URL: http://surgpathcriteria.stanford.edu/breast/dcis/apocrinedcis.html. Accessed on: 4 August 2011.
- ↑ URL: http://surgpathcriteria.stanford.edu/breast/dcis/. Accessed on: 4 August 2011.
- ↑ O'Malley, Frances P.; Pinder, Sarah E. (2006). Breast Pathology: A Volume in Foundations in Diagnostic Pathology series (1st ed.). Churchill Livingstone. pp. 168. ISBN 978-0443066801.
- ↑ Tadrous, Paul.J. Diagnostic Criteria Handbook in Histopathology: A Surgical Pathology Vade Mecum (1st ed.). Wiley. pp. 258. ISBN 978-0470519035.
- ↑ Lara, JF.; Young, SM.; Velilla, RE.; Santoro, EJ.; Templeton, SF. (Nov 2003). "The relevance of occult axillary micrometastasis in ductal carcinoma in situ: a clinicopathologic study with long-term follow-up.". Cancer 98 (10): 2105-13. doi:10.1002/cncr.11761. PMID 14601079.
- ↑ Broekhuizen, LN.; Wijsman, JH.; Peterse, JL.; Rutgers, EJ. (Jun 2006). "The incidence and significance of micrometastases in lymph nodes of patients with ductal carcinoma in situ and T1a carcinoma of the breast.". Eur J Surg Oncol 32 (5): 502-6. doi:10.1016/j.ejso.2006.02.006. PMID 16569492.
- ↑ Weedman Molavi, Diana (2008). The Practice of Surgical Pathology: A Beginner's Guide to the Diagnostic Process (1st ed.). Springer. pp. 188. ISBN 978-0387744858.
- ↑ 18.0 18.1 O'Malley, Frances P.; Pinder, Sarah E. (2006). Breast Pathology: A Volume in Foundations in Diagnostic Pathology series (1st ed.). Churchill Livingstone. pp. 170. ISBN 978-0443066801.