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Definition of cytopathology
Cytopathology is the study of normal and abnormal
exfoliated cells in tissue fluid.
The individual cells reflect the normal and abnormal
morphology of the tissue from which they are derived.
Types of exfoliated cyto-pathology
Natural spontaneous exfoliation
Natural covering epithelium: skin, urinary tract, vagina, and
cervix.
Glandular epithelial secretion: Breast (Nipple secretion).
Sputum
Urine
Exudates and transudate:
Pleural fluid Peritoneal fluid
Pericardial fluid Joint fluid CSF
Artificial enhanced exfoliation:
Scrapings from cervix, vagina, oral cavity, and skin
Brushing and lavage: bronchi, GIT, and urinary tract
Fine needle aspiration (FNA) for:
Body cavity fluid: pleural, pericardial & peritoneal
fluids
Cysts: neck, breast & ovary
Solid tissue: body organs, tumors & other swell
Role of cytopathology
Early detection of unsuspected diseases (malignant
or pre-malignant lesions).
Confirmation of suspected diseases without surgical
trauma.
Diagnosis of hormonal imbalance.
Useful in flow up the course of disease or
monitoring therapy.
Advantage of Cytopathology
Rapid diagnosis - Inexpensive - Simple
It is better in evaluating the infectious diseases.
Supplement or replace frozen section or biopsy
No injury to tissue allowing repeated sampling
It is better for hormonal assay
Cytopathological smear cover a wider surface than
that involved in surgical biopsy.
Disadvantage of Cytopathology
Interpretation of the morphological cellular changes is
based only on individual cell observation.
Not always finally diagnosis, so it is confirmed by
histopathology in some cases.
Not determine the size and type of lesion of some cases.
Factors that determine the appearance of
cells
Type of the technique used.
Level of cell maturation at the time of cell collection.
Nature of the parents tissue: soft tissue, cyst, or solid organ.
Medium of the exfoliated cells.
Interval between the stain of the exfoliated cells and collection
of samples.
Type of fixative, stain, and processing of the technique
used.
PAP smear: named after
Dr. George Papanicolaou (1883-1962)
Vaginal smears from guinea pigs (1917)
Women (1920)
Hormonal cycles
Pathological conditions (1928)
Normal Cervix
Taking the Sample
Liquid Based Cytology – lab processing
Cytologic screening for cervical cancer
Cervical cancer screening has decreased morbidity and
mortality
Deaths from cervical cancer decreased from 26,000 to
less than 5,000 between 1941 and 1997
Pap smears are not perfect
For a high grade lesion, the sensitivity of a single pap
smear is only 60-80%
Estimated false negative rate is 30-50%
Requires adequate specimen collection
Requires adequate cytological review
Requires adequate patient and physician follow-up
10% of women with cervical cancer had inappropriate
follow-up.
Requires access to care
50% of women with cervical cancer were never
screened and 10% had not been screened within 5 years
of diagnosis.
Who to screen
Any woman with a cervix who has ever had sexual
activity.
When to screen
Start within 3 years of onset of sexual activity or by age
of 21, whichever is first.
Risk factors for cervical dysplasia
Early onset of sexual activity
Multiple sexual partners
Tobacco
Oral contraceptives
Screening frequency
Yearly until three consecutive normal pap smears, then
may decrease frequency to every three years
Annual screening for high-risk women is highly
recommend.
When to stop routine screening
Age 65 and “adequate recent screening”
Three consecutive normal pap smears
No abnormal pap smears in last 10 years
No history of cervical or uterine cancer
Hysterectomy for benign disease
Hysterectomy for invasive cervical cancer
Original Squamous Epithelium
Vagina and outer ectocervix
4 cell layers
Well-glycogenated (pink) unless atrophic
Columnar Epithelium
Upper and middle endo-cervical canal
Single layer of columnar cells arranged in
folds
Mucin producing (not true glands)
Squamous Metaplasia
Central ectocervix and proximal endocervical canal
Replacement of columnar cells by squamous epithelium
Progressive and stimulated by
Acidic environment with onset of puberty
Estrogen causing eversion of endocervix
Transformation Zone
Zone between original squamo-columnar junction and
the “new” squamo-columnar junction
Nabothian cysts visually identify the transformation
zone if present
Original Squamo-columnar Junction
Placement determined between 18-20 weeks gestation
Most often found on ectocervix
Can be found in vagina or vaginal fornices
Less apparent over time with maturation of
epithelium
“New” Squamo-columnar Junction
Border between squamous epithelium and columnar
epithelium
Found on ecto-cervix or in endo-cervical canal
Majority of cervical cancers and precursor lesions
arise in immature squamous metaplasia, i.e. the
leading edge of the squamo-columnar junction
Squamous Epithelium
Parabasal Cells
Intermediate Cells
Superficial Cells
Endocervix
Endocervical Cells
Endometrial Cells
Non-Epithelial Cells
sperms
Lymphocytes Polymorphs
Normal smear
Ectropion / Erosion
At puberty & pregnancy the endocervical cells are
pushed out to lie on the ectocervix
Normal Ectropion
Wide Ectropion
Metaplasia
The endocervical cells are transformed into squamous
cells through the process of squamous metaplasia
Metaplastic Cells

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1-introductionofcytopathology-170421144339.pdf

  • 1.
  • 2. Definition of cytopathology Cytopathology is the study of normal and abnormal exfoliated cells in tissue fluid. The individual cells reflect the normal and abnormal morphology of the tissue from which they are derived.
  • 3. Types of exfoliated cyto-pathology Natural spontaneous exfoliation Natural covering epithelium: skin, urinary tract, vagina, and cervix. Glandular epithelial secretion: Breast (Nipple secretion). Sputum Urine Exudates and transudate: Pleural fluid Peritoneal fluid Pericardial fluid Joint fluid CSF
  • 4. Artificial enhanced exfoliation: Scrapings from cervix, vagina, oral cavity, and skin Brushing and lavage: bronchi, GIT, and urinary tract Fine needle aspiration (FNA) for: Body cavity fluid: pleural, pericardial & peritoneal fluids Cysts: neck, breast & ovary Solid tissue: body organs, tumors & other swell
  • 5. Role of cytopathology Early detection of unsuspected diseases (malignant or pre-malignant lesions). Confirmation of suspected diseases without surgical trauma. Diagnosis of hormonal imbalance. Useful in flow up the course of disease or monitoring therapy.
  • 6. Advantage of Cytopathology Rapid diagnosis - Inexpensive - Simple It is better in evaluating the infectious diseases. Supplement or replace frozen section or biopsy No injury to tissue allowing repeated sampling It is better for hormonal assay Cytopathological smear cover a wider surface than that involved in surgical biopsy.
  • 7. Disadvantage of Cytopathology Interpretation of the morphological cellular changes is based only on individual cell observation. Not always finally diagnosis, so it is confirmed by histopathology in some cases. Not determine the size and type of lesion of some cases.
  • 8. Factors that determine the appearance of cells Type of the technique used. Level of cell maturation at the time of cell collection. Nature of the parents tissue: soft tissue, cyst, or solid organ. Medium of the exfoliated cells. Interval between the stain of the exfoliated cells and collection of samples. Type of fixative, stain, and processing of the technique used.
  • 9. PAP smear: named after Dr. George Papanicolaou (1883-1962) Vaginal smears from guinea pigs (1917) Women (1920) Hormonal cycles Pathological conditions (1928)
  • 12.
  • 13. Liquid Based Cytology – lab processing
  • 14.
  • 15. Cytologic screening for cervical cancer Cervical cancer screening has decreased morbidity and mortality Deaths from cervical cancer decreased from 26,000 to less than 5,000 between 1941 and 1997
  • 16. Pap smears are not perfect For a high grade lesion, the sensitivity of a single pap smear is only 60-80% Estimated false negative rate is 30-50% Requires adequate specimen collection Requires adequate cytological review
  • 17. Requires adequate patient and physician follow-up 10% of women with cervical cancer had inappropriate follow-up. Requires access to care 50% of women with cervical cancer were never screened and 10% had not been screened within 5 years of diagnosis.
  • 18. Who to screen Any woman with a cervix who has ever had sexual activity.
  • 19. When to screen Start within 3 years of onset of sexual activity or by age of 21, whichever is first. Risk factors for cervical dysplasia Early onset of sexual activity Multiple sexual partners Tobacco Oral contraceptives
  • 20. Screening frequency Yearly until three consecutive normal pap smears, then may decrease frequency to every three years Annual screening for high-risk women is highly recommend.
  • 21. When to stop routine screening Age 65 and “adequate recent screening” Three consecutive normal pap smears No abnormal pap smears in last 10 years No history of cervical or uterine cancer Hysterectomy for benign disease Hysterectomy for invasive cervical cancer
  • 22.
  • 23. Original Squamous Epithelium Vagina and outer ectocervix 4 cell layers Well-glycogenated (pink) unless atrophic
  • 24. Columnar Epithelium Upper and middle endo-cervical canal Single layer of columnar cells arranged in folds Mucin producing (not true glands)
  • 25. Squamous Metaplasia Central ectocervix and proximal endocervical canal Replacement of columnar cells by squamous epithelium Progressive and stimulated by Acidic environment with onset of puberty Estrogen causing eversion of endocervix
  • 26. Transformation Zone Zone between original squamo-columnar junction and the “new” squamo-columnar junction Nabothian cysts visually identify the transformation zone if present
  • 27. Original Squamo-columnar Junction Placement determined between 18-20 weeks gestation Most often found on ectocervix Can be found in vagina or vaginal fornices Less apparent over time with maturation of epithelium
  • 28. “New” Squamo-columnar Junction Border between squamous epithelium and columnar epithelium Found on ecto-cervix or in endo-cervical canal Majority of cervical cancers and precursor lesions arise in immature squamous metaplasia, i.e. the leading edge of the squamo-columnar junction
  • 38. Ectropion / Erosion At puberty & pregnancy the endocervical cells are pushed out to lie on the ectocervix Normal Ectropion
  • 40. Metaplasia The endocervical cells are transformed into squamous cells through the process of squamous metaplasia