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Thanaa Helal Professor of Pathology Faculty of Medicine – Ain Shams University.

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Presentation on theme: "Thanaa Helal Professor of Pathology Faculty of Medicine – Ain Shams University."— Presentation transcript:

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3 Thanaa Helal Professor of Pathology Faculty of Medicine – Ain Shams University.

4 Proliferation Differentiation

5 According to Behaviour Benign Locally malignant Malignant  Basal cell Ca  Craniophayngioma  Amelablastoma  Giant cell tumor  Basal cell Ca  Craniophayngioma  Amelablastoma  Giant cell tumor

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7  Increased N/C ratio  Nuclear pleomorphism  Nuclear hyperchromatism  Prominent nucleoli  Irregular nuclear membrane  Abnormal mitotic figures  Increased N/C ratio  Nuclear pleomorphism  Nuclear hyperchromatism  Prominent nucleoli  Irregular nuclear membrane  Abnormal mitotic figures

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9 Differences Between Benign and Malignant Tumours BenignMalignant Size SmallLarge Capsule +- Similarity to tissue of origin +- Criteria of malignancy -+ Rate of growth SlowRapid Mode of growth CompressionInfiltration Spread -+ DNA pattern DiploidAneuploid

10 Malignant (Leiomyosarcoma) Benign (Leiomyoma)

11 Epithelial Mesenchymal Benign Malignant Benign Malignant Carcinoma Sarcoma

12 Differences between carcinoma and sarcoma CarcinomaSarcoma Origin EpitheliumConnective tissue Age More in oldMore in young Vascularity Less vascularMore vascular Rate of growth Less rapidMore rapid Cut section Less hgeMore hge Spread Early by lymphatics Early by blood Prognosis Less worseMore worse Microscopic Cells arranged in groups Cells arranged individually

13 Carcinoma Sarcoma

14 Epithelial Tumours BenignMalignant 1. Squamous epithelium S. cell papillomaS. cell carcinoma 2. Basal cells of skin ---Basal cell carcinoma 3. Melanocytes NaevusMalignant melanoma 4. Glandular epithelium Adenoma (Cystadenoma) Adenocarcinoma (Cystadenocarcinoma) 5. Transitional epithelium T.cell papillomaT.cell carcinoma 6. Trophoblastic epithelium Vesicular moleChoriocarcinoma

15 1) Papilloma  Gross: Sessile or pedunculated polypoid mass 1) Papilloma  Gross: Sessile or pedunculated polypoid mass Precancerous

16  Microscopic: A central core of connective tissue covered by epithelium which may be A)Squamous: Skin, upper resp. tract, upper GIT  Microscopic: A central core of connective tissue covered by epithelium which may be A)Squamous: Skin, upper resp. tract, upper GIT

17 B)Transitional: UB, ureter, renal pelvis

18 2.Junctional naevus: Dermoepidermal junction 2.Junctional naevus: Dermoepidermal junction

19 3.Compound naevus: Both dermis and DEJ

20 C)Columnar: Duct papilloma of the breast

21 2) Adenoma, Arises from: A. Mucous membrane: GIT, Bronchi, Breast, Ovary B. Endocrine glands: Thyroid, adrenal Gross A)Endocrine glands: Encapsulated mass B) GIT: Adenomatous polyp (Precancerous) C) Ovary: Cystadenoma, Papillary cystadenoma D) Breast: Fibroadenoma 2) Adenoma, Arises from: A. Mucous membrane: GIT, Bronchi, Breast, Ovary B. Endocrine glands: Thyroid, adrenal Gross A)Endocrine glands: Encapsulated mass B) GIT: Adenomatous polyp (Precancerous) C) Ovary: Cystadenoma, Papillary cystadenoma D) Breast: Fibroadenoma (Precancerous) Microscopic: Similar to normal tissue

22 Encapsulated mass Papillary cystadenoma Fibroadenoma Polyp Adenoma

23 GrossGross InfiltratingInfiltrating Fungating UlcerativeUlcerative

24 Microscopic  Squamous cell carcinoma  Transitional cell carcinoma  Adenocarcinoma  Basal cell carcinoma Microscopic  Squamous cell carcinoma  Transitional cell carcinoma  Adenocarcinoma  Basal cell carcinoma

25 Site  Surfaces originally covered by sq. epith. as: skin, upper resp. tract and upper GIT  Surfaces covered by any epith. after sq. metaplasia as: bladder, bronchi, cervix Gross  Fungating mass  Malignant ulcer Site  Surfaces originally covered by sq. epith. as: skin, upper resp. tract and upper GIT  Surfaces covered by any epith. after sq. metaplasia as: bladder, bronchi, cervix Gross  Fungating mass  Malignant ulcer

26 Microscopic  Masses of squamous epithelium with central keratin (cell nests) Grading: Broder’s classification  Grade 1 : > 50% cell nests  Grade 2 : 25-50% cell nests  Grade 3 : < 25% cell nests Spread: Direct, Lymphatic, Blood Microscopic  Masses of squamous epithelium with central keratin (cell nests) Grading: Broder’s classification  Grade 1 : > 50% cell nests  Grade 2 : 25-50% cell nests  Grade 3 : < 25% cell nests Spread: Direct, Lymphatic, Blood

27 Well diff. SCC: grade I Poorly diff. SCC: grade III

28 Site: Face Gross  Early: Papule  Late: Rodent ulcer Site: Face Gross  Early: Papule  Late: Rodent ulcer

29 Microscopic  Infiltration of the dermis by masses of basaloid cells (oval with dark nuclei and minimal basophilic cytoplasm)  Peripheral palisading Microscopic  Infiltration of the dermis by masses of basaloid cells (oval with dark nuclei and minimal basophilic cytoplasm)  Peripheral palisading

30 Spread  Local spread only  Lymphatic spread: Only in case of  Secondary infection  Squamous Ca + Basal CC  Blood spread: Never Spread  Local spread only  Lymphatic spread: Only in case of  Secondary infection  Squamous Ca + Basal CC  Blood spread: Never

31 (1) Classic adenocarcinomas  Site: As adenoma  Gross: (1) Classic adenocarcinomas  Site: As adenoma  Gross: InfiltratingInfiltrating Fungating UlcerativeUlcerative

32  Microscopic: Malignant acini + solid masses  Grading Grade 1 : > 50% acini Grade 2 : 25 - 50% acini Grade 3 : <25% acini  Microscopic: Malignant acini + solid masses  Grading Grade 1 : > 50% acini Grade 2 : 25 - 50% acini Grade 3 : <25% acini

33 (2) Mucoid carcinoma  Site : Stomach, large intestine, breast  Gross: Soft and gelatinous mass  Microscopic: Lakes of mucin containing malignant cells (2) Mucoid carcinoma  Site : Stomach, large intestine, breast  Gross: Soft and gelatinous mass  Microscopic: Lakes of mucin containing malignant cells

34 (3) Signet ring carcinoma  Site : Stomach, large intestine  Gross: Diffusely infiltrating lesion  thickening of wall of stomach or large intestine  Microscopic: Diffuse infiltration by signet ring cells (3) Signet ring carcinoma  Site : Stomach, large intestine  Gross: Diffusely infiltrating lesion  thickening of wall of stomach or large intestine  Microscopic: Diffuse infiltration by signet ring cells

35  Benign: Naevus (benign melanoma)  Gross Size: Small Shape: Rounded Consistency: Firm Capsule: Not encapsulated, well circumscribed well circumscribed Cut section: Brownish  Benign: Naevus (benign melanoma)  Gross Size: Small Shape: Rounded Consistency: Firm Capsule: Not encapsulated, well circumscribed well circumscribed Cut section: Brownish

36  Microscopic 1.Intradermal naevus: Dermis only 1.Intradermal naevus: Dermis only

37 Risk factors  Sun exposure  Fair skin  Nevus  Rapid growth  Increased pig.  Ulceration Site: Face, neck, chest Risk factors  Sun exposure  Fair skin  Nevus  Rapid growth  Increased pig.  Ulceration Site: Face, neck, chest

38 Gross  Size : Small  Shape: Rounded  Consistency: firm  Capsule: non-encapsulated and infiltrating adjacent and infiltrating adjacentstructures  Cut section: Brownish Gross  Size : Small  Shape: Rounded  Consistency: firm  Capsule: non-encapsulated and infiltrating adjacent and infiltrating adjacentstructures  Cut section: Brownish

39 Microscopic 1- In situ malignant melanoma: Intraepidermal pagetoid spread Microscopic 1- In situ malignant melanoma: Intraepidermal pagetoid spread

40 Microscopic 2- Invasive malignant melanoma  Diffuse infiltration of the dermis by malignant melanocytes which are epithelial or spindle-shaped and usually contain melanin Microscopic 2- Invasive malignant melanoma  Diffuse infiltration of the dermis by malignant melanocytes which are epithelial or spindle-shaped and usually contain melanin

41 Site  Original epith. as: skin, bladder, breast, cervix  Metaplastic epith.: bladder, bronchus, cervix Gross  Rough paplular areas  Superficial ulceration Site  Original epith. as: skin, bladder, breast, cervix  Metaplastic epith.: bladder, bronchus, cervix Gross  Rough paplular areas  Superficial ulceration

42 Microscopic  Criteria of malignancy in the whole thickness of epithelium with intact basement membrane  Later on: invasion of BM  invasive carcinoma Microscopic  Criteria of malignancy in the whole thickness of epithelium with intact basement membrane  Later on: invasion of BM  invasive carcinoma

43 Mesenchymal Tumours (Soft tissue tumours) Mesenchymal Tumours (Soft tissue tumours) BenignMalignant 1. Fibrous tissue FibromaFibrosarcoma 2. Fatty tissue (lipocytes) LipomaLiposarcoma 3. Smooth m. (leios) LeiomyomaLeiomyosarcoma 4. Striated m. (Rhabdos) RhadomyomaRhabdomyosarcoma 5. Blood vessels HaemangiomaAngiosarcoma 6. Lymph vessels LymphangiomaLymphangiosarcoma 7. Cartilage (Chondrocytes) ChondromaChondrosarcoma 8. Bone (osteoid) OsteomaOsteosarcoma 9. Mesothelium B. mesotheliomaM. mesothelioma 10. Lymphoid tissue ---Lymphoma.

44  Benign: Fibroma  Site: Any area of fibrous tissue  Gross  Size: variable  Shape: Rounded or oval  Consistency: Firm  Capsule: present  Cut section : Whitish  Benign: Fibroma  Site: Any area of fibrous tissue  Gross  Size: variable  Shape: Rounded or oval  Consistency: Firm  Capsule: present  Cut section : Whitish

45  Microscopic Parallel bundles of spindle-shaped fibroblasts  Microscopic Parallel bundles of spindle-shaped fibroblasts

46  Site: Mainly in the extremities  Gross Size: variable Shape: rounded or oval Consistency: firm Capsule: may be encapsulated encapsulated Cut section: whitish  Site: Mainly in the extremities  Gross Size: variable Shape: rounded or oval Consistency: firm Capsule: may be encapsulated encapsulated Cut section: whitish


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