Uterine cervix
The cervix, or uterine cervix to be more precise, is the gateway to the uterine corpus. It is not infrequently afflicited by cancer -- squamous cell carcinoma. Prior to routinue pap tests it was a leading cause of cancer death in women in the Western world. Polyps associated with the cervix are disussed the cervical polyp article.
Introduction
- Consists of non-keratinized squamous epithelium and simple columnar epithelium.
- The area of overlap (between squamous & columnar) is known as the "transformation zone".[1]
- Also known as "transition zone".
- Most cervix cancer is squamous cell carcinoma.
Common benign
Nabothian cyst:
- Simple endocervical cyst.
- Lined by endocervical epithelial cells.
- Columnar morphology with large clear, apical vacuoles.
- Lined by endocervical epithelial cells.
Tunnel cluster:
- Benign proliferation of endocervical glands[2]
- Important only as one could mistake minimal deviation adenocarcinoma for it.
Where to start
- Identify epithelium - exocervical (stratified squamous), endocervical (simple columnar), both.
- If there is both exocervix and endocervix --> transition zone.
- Identify possible squamous lesions.
- Identify possible endocervical lesions.
Endocervical glands
Cervical glands normally have round nuclei and vaguely resemble the colonic mucosa.
- If the nuclei are columnar think cancer! This is like in the colon-- columnar nuclei = badness.
Mnemonic: The Cs (Cervix & Colon) are similar.
Cervical intraepithelial neoplasia (CIN)
Refers to changes in squamous epithelium.
Grades (squamous intraepithelial neoplasia):
- CIN I = mild dysplasia.
- CIN II = moderate dysplasia.
- CIN III = severe dysplasia.
Bethesda system:
- LSIL (low-grade squamous intraepithelial lesion) = CIN I.
- HSIL (high-grade squamous intraepithelial lesion) = CIN II, CIN III.
Treatment
- LSIL: nothing, as usually regress.
- HSIL: excision (e.g. cone, LEEP, laser) + followup.
LEEP = Loop Electrosurgical Excision Procedure (LEEP) Procedure.
- Used for squamous lesions -- pathologist typically gets several pieces.
Cone
- Used for endocervical lesions, i.e. adenocarcinoma in situ (AIS).
- Pathologist gets a ring or donut-shaped piece of tissue.
Histologic changes in CIN I, CIN II and CIN III
- CIN I = cytoplasmic halos (koilocytic atypia), atypical cells close to basement membrane only.
- CIN II = increased nuclear-cytoplasmic ratio, loss of polarity, incr. mitoses, hyperchromasia.
- If there are large nuclei... you should seen 'em on low power, i.e. 25x.
- CIN III = same changes as in CIN II + outer third (or full thickness).
Ref.:[5]
Notes:
- Hyperchromasia is a very useful feature for identifying CIN (particularily at low power, i.e. 25x).
- Kiolocytes are the key feature of CIN I.
- Kiolocytes are not considered to be part of a CIN II lesion or CIN III lesion.
- Large irregular nuclei are not required for CIN II... but you should think about it.
- Some mild changes at the squamo-columnar junction are expected.
- Look for the location of mitoses...
- If there is a mitosis in the inner third (of the epithelial layer) = at least CIN I.
- If there is a mitosis in the middle third (of the epithelial layer) = at least CIN II.
- If there is a mitosis in the outer third = CIN III.
- Nucleoli are usually NOT present in CIN.[6]
- Nucleoli are common in reactive changes.[7]
Kiolocytes versus benign squamous
Kiolocytes:
- Perinuclear clearing.
- Nuclear changes.
- Size similar (or larger) to those in the basal layer of the epithelium.
- Nuclear enlargement should be evident on low power, i.e. 25x. [8]
- Central location - nucleus should be smack in the middle of the cell.
Notes:
- Both perinuclear clearing and nuclear changes are essential.
- Benign cells have a small nucleus that is peripheral.
Cervix cancer grading
- Well-differentiated (keratinizing).
- Moderately diff. (nonkeratinizing).
- Poorly differentiated.
Ref.:[9]
SCC of the cervix versus CIN III
Invasive cancer look for:
- Eosinophilia.
- Extra large nuclei, i.e. nuclei 5x normal size.
- Stromal inflammation (lymphocytes, plasma cells).
- Long rete ridges.
- Numerous beeds/blobs of epithelial cells that seem unlikely to be rete ridges.
- Desmoplastic stroma - increased cellularity, spindle cell morphology[10]
Pitfalls:
- Squamous metaplasia
- If you can trace the squamous cells from a gland to the surface it is less likely to be invasive cancer
See: http://www.nature.com/modpathol/journal/v15/n3/pdf/3880520a.pdf
Squamous metaplasia
Squamous metaplasia is a response to inflammation...
- Nuclei are uniform size and round.
- Intercellular bridges are often seen/edema is often seen.
- Uniform cell spacing, i.e. NO crowding.
- NEGATIVES
- No mitoses (think cancer/CIN if you see 'em)
- Usually no hyperchromatism (think cancer/CIN if you see it)
Notes:
- It is possible to confuse CIN III with squamous metaplasia.
IHC:
- p16 (poor man's test for HPV).
- Ki-67 (proliferation marker).
Adenocarcinoma
- Adenocarcinoma of the cervix/adenocarcinoma in situ (AIS) of the cervis is much less common than squamous dysplasia of the cervix/SCC of the cervix.
- AIS/adenocarcinoma arises can arise from the endocervical glands.
AIS
- Diagnosis of AIS dependent primarily on nuclear changes:[11]
- Nuclear crowding.
- Nuclear hyperchromasia.
- Cigar-shaped nuclei.
- +/-Mitoses.
- Cytoplasm.
- Hyperchromasia.
Invasive
- Invasive adenocarcinoma
- May be difficult to be certain.
- Stromal changes - "desmoplastic stroma/desmoplastic reaction".
- Fibrosis/streaming cells.
- Gland fusion.
- Glands too deep -- very fuzzy criterion.
Notes:
- AIS changes - similar to colonic dysplasia.
- AIS may occur together with CIN.
- not infrequently they (AIS, CIN) occur together - both are due, indirectly, to HPV infection.
IHC
Uterus vs. cervix[12]
- Cervix (typically): CEA+, p16+
- ... and ER-, PR-, vimentin-
- Uterus (typically): vimentin+, ER+, PR+
- ... and CEA-, p16-
See also
References
- ↑ URL: http://www.med-ed.virginia.edu/Courses/path/gyn/cervix1.cfm. Accessed on: 12 May 2010.
- ↑ http://pathologyoutlines.com/cervix.html#tunnelclusters
- ↑ [need ref]
- ↑ [need ref]
- ↑ PBoD P.1075-6.
- ↑ STC. Jan 2009.
- ↑ STC. Jan 2009.
- ↑ V. Dube 2008.
- ↑ PBoD P.1077.
- ↑ NEED REF.
- ↑ need ref
- ↑ LAE 15 Jan 2009.