Neoplasia I: Definition and Classification

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    • What is neoplasia?
      Abnormal mass of tissue, the growth of which is uncoordinated with that of normal tissues and persists after the stimulus is removed
    • What is a tumour?

      Swelling, generally without inflammation, caused by an abnormal growth of tissue whether benign or malignant
    • What are the major categories for cell types of origin for tumours?
      Epithelium
      Connective tissue
      Lymphoid/haematopoietic tissue
      Germ cells
    • What is tumour differentiation?
      Tumour differentiation refers to how well the tumour resembles its normal counterpart, both morphologically & functionally
    • Are well differentiated lesions more or less proliferative than the poorly differentiated ones?
      Generally, they are less proliferative & less aggressive, with less potential for metastatic spread than their poorly differentiated counterparts
      There are exceptions
    • What are the different grades of tumours?
      Grade 1/well differentiated
      Grade 2/moderately differentiated
      Grade 3/poorly differentiated
    • What are some important definitions regarding abnormalities of growth & can you give examples of each one?
      Hyperplasia: Bone marrow cells in people living at high altitudes
      Hypertrophy: Bodybuilders/athletes
      Atrophy: Muscle atrophy in a dis-used limb
      Involution: Breast tissue on cessation of breastfeeding
      Metaplasia: Barrett’s oesophagus
      Dysplasia: Cervical screening
    • How do you differentiate benign neoplasia from malignant neoplasia?
      Benign:Well differentiated, likely to resemble tissue of originSlow growthMitotic figures rare and normalWell demarcatedExpansible growthDo not metastasise
      Malignant:Spectrum of differentiation from well to poorly differentiatedGrowth rate variable and less predicableMitotic figures may be numerous and atypicalPoorly demarcatedLocally invasiveRegional and distant metastasis
      Metastasise = Spread to other parts of the body
    • Which tumours are more common?
      Epithelial2 multiple choice options
    • What are the general rules for tumour nomenclature?
      Generally speaking forepithelial tumours, if the suffix is carcinoma it's malignant and if it's papilloma or adenoma, it's benign
      Formesenchymal tumours, if the suffix is sarcoma, it's malignant and if it's just -oma, then it's benign
      The prefix of the tumour will always refer to the type of tissue of origin e.g. osteoma (osteo meaning bone)
    • What are some individual tumour names we should be familiar with?
      Lymphoma- malignant tumours of the lymphoid system
      Melanoma- malignant tumour of melanocytes
      Leukaemia- malignant tumour of bone marrow cells
      Teratoma- a tumour which includes elements of all 3 embryonic germ layers
      Hamartoma- a developmental anomaly (not actually a tumour)
    • What can cause tumours?
      Genetic predisposition, surrounding tissues e.g. inflammation, environmental/social/infectious factors

      Some cancers can also be caused by viruses and infection
    • What are the different ways that malignant tumours spread?
      Direct- local infiltration
      Lymphatic- to regional lymph nodes
      Haematogenous- lungs, liver, bone
      Peri-neural-salivary tumours
      Trans-coelomic- pleura, pericardium, peritoneal
    • What forms the lining of the oral mucosa?
      Squamous epithelium
    • How do squamous cells infiltrate & become malignant cells?
      They undergo genetic changes & lose those tight attachments to each other

      They disrupt/dissolve the basement membrane & then they gain the ability to enter connective tissues and acquire mobility
    • What are the sequence of events that makes it go from a primary to a metastatic tumour?
      Tumour cells secrete vascular growth factors- encouragesangiogenesis (formation of new blood vessels)
      Well vascularised tumour has good supply of nutrients & oxygen so can keep growing at an abnormal rate
      Large sheets of tumour cellsdetachby downregulating proteins that normally mediate their connections
      Then,invasion of connective tissuestowards blood vessels & lymphatic channels happens and this involves acquiring mobility
      Evasion of host defencesfollows
      Then,migration through vessel wall& aformation of a tumour embolushappens as well asfurther evasion of host defences
      Next we haveadhesion to vessel wall, and they can utilise processes very similar to inflammatory cellextravasationto gain access to the tissues
      Finally, there isinvasion of new host tissue&angiogenesisagain
    • What are some non-malignant effects of tumours?
      Increased tendency to thrombosis
      Cellular overactivity
      Paraneoplastic phenomenon -set signs and symptoms that are a consequence of the presence of the tumour but not directly attributable to it.
    • What are some factors that affect prognosis of tumours?
      Tumour type
      Site and size; resectability
      Differentiation
      Degree of cellular atypia (cellular state of not being typical)
      Depth and extent of invasion
      Mitotic index and degree of mitotic atypia
      Regional lymph node involvement
      Distant metastasis
    • What prognostic index is used for melanoma?
      Clark Levels (level 1 being the least invasive and level 5 being the most)
    • What prognostic index is used for colorectal cancer?
      Dukes staging:

      Dukes A being confined to the bowel wall whereas Dukes D is distant metastases
    • What prognostic index can we use for histological images?
      Mitotic count,
    • How do you diagnose a tumour?
      You need a tissue sample for diagnosis of presence of a tumour and also to sub-type it

      Radiology can help to define size, extent and structures involved and might give some clues as to the tumour type Tissue:

      -Fine needle aspirate (FNA)
      -Histology (biopsy)
    • What is screening?
      The systematic search for cancer in people who have no signs or symptoms of cancer
    • What are a couple of issues with screening?
      False positives
      Over diagnosis e.g some people with papillary thyroid cancer are not affected at all during their lifetime
    • Why is screening common for cervical, breast, & colorectal cancer but not for lung, thyroid, & prostate cancer?
      Lung:CT screening 70-90% patients had 1 false positive result–remember radiological examination does not diagnose cancer and consider the radiation dose for a CT chest
      Prostate: PSA screening 25-30% of patients had 1 false positive result–equally a simple blood test cannot differentiate a hyperplastic prostate from a malignant one
    • What is the difference between staging and grading?
      Gradingis tumour differentiation (well, moderate, poor)
      Staginguses aT N Mclassification (T-tumour;N-lymph nodes;M-metastasis) and it's all about prognosis
    • Questions to answer:
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