Fundamentals of tumours Flashcards

1
Q

Compare and contrast benign and malignant tumours (macroscopic and microscopic)

A

Benign
• slower growing
• well circumscribed
• often encapsulated by a layer of compressed fibrous tissue
• not locally invasive (although the tumour may push and compress the adjacent normal tissue as it increases in size)
• no metastatic potential
• tumour cells very closely resemble cell of origin ie. very well differentiated
• cells are uniform throughout the tumour
• few mitoses
• tumour cells have a normal nuclear:cytoplasmic ratio

Malignant (‘cancer’)
• faster growing
• poorly circumscribed
• non-encapsulated
• INVASIVE GROWTH with destruction of adjacent normal tissue
• METASTATIC POTENTIAL
• may or may not closely resemble cell of origin ie. variable differentiation
• cells and nuclei vary in shape and size (pleomorphism)
• many mitoses
• high nuclear:cytoplasmic ratio.
• nuclear staining (hyperchromatism)

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2
Q

Define tumour grade and stage

A

Grading

  • the grade reflects how closely it resembles (down the microscope) the normal tissue from which it is believed to have arisen ie. it is an assessment of differentiation:
  • well differentiated: the cancer cells closely resemble the normal tissue.
  • poorly differentiated: the cancer cells poorly resemble the normal tissue.
  • correlates with aggressiveness of behaviour

Staging

  • staging is the process of determining how much cancer there is the body and where it is located ie. it provides a quantitative assessment of the extent of anatomical spread by tumour
  • TNM
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3
Q

Define dysplasia- hint: broad definition, classification and basement membrane

A

Dysplasia may be defined as ‘disordered growth or differentiation’.

Dysplasia is characterised microscopically by varying degrees of decreased differentiation, more mitoses, high nuclear:cytoplasmic ratio, cellular/nuclear pleomorphism.

the cells have not yet invaded through the basement membrane.

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4
Q

Explain why it is preferable to treat a patient with precancer rather than cancer

A

removing a precancerous lesion with a clear margin around it should be curative.

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5
Q

What is lined by each type of epithelium?

  • squamous epithelium
  • glandular epithelium
  • urothelium/ transitional epithelium
A
  • squamous epithelium eg. skin and oesophagus, anus
  • glandular epithelium eg. respiratory and gastrointestinal tracts.
  • urothelium (old term - transitional epithelium) eg. urinary tract.
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6
Q

Explain how tumour grade and stage differ from one another

A

Stage: extent of anatomical spread. Grade: aggressiveness of behaviour.

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7
Q

Give examples of grading and staging systems used in clinical practice (3)- hint gynae cancers, lymphoma, CRC

A
  • FIGO system is used for gynaecological cancers.
  • Ann Arbor system is used for lymphomas.
  • Dukes’ system is oden used for colorectal carcinoma (in addition to TNM staging).
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8
Q

Explain the concept of premalignancy (precancer).

A

Precancer does not show invasive growth and does not have the ability to metastasise

Dysplasia/ carcinoma in situ

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9
Q

4 reasons we stage cancer

A

• stage is usually the single most important prognostic factor for a cancer.
[Prognostic factors are factors which help predict the probable course and outcome of a disease].
• knowing the stage helps in planning the most appropriate treatment.
• staging provides a common language with which doctors can communicate about a patient.
• knowing the stage is important in identifying clinical trials that may be suitable for a particular patient

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10
Q

Give examples of the different terminology used for premalignancy in different anatomical sites

A

Cervix- Cervical Intraepithelial Neoplasia
Endometrium- Atypical Hyperplasia
Bladder- Carcinoma In Situ
Prostate- Prostatic Intraepithelial Neoplasia
Colorectum- Low and High Grade Dysplasia
Breast- Ductal Carcinoma In Situ
Skin- Actinic Keratosis

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11
Q

Outline the rationale for the breast, cervical and bowel cancer screening programmes

A

One of the main aims of the national breast, colon and cervical screening programmes is to detect and treat precancer.

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12
Q

5 common sites for metastasis

A
Lung
Liver
Brain
Bone marrow
Bone
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13
Q

5 effects of cancer metastasis at the common sites

A

Lung: Haemoptysis, pneumonia, pleural effusion
Liver: Jaundice, hepatic failure
Brain: Seizures, stroke
Bone marrow: Anaemia, leukopaenia, thrombocytopaenia
Bone: Pain, fracture, spinal cord compression

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14
Q

Define paraneoplastic syndrome

A

a syndrome (ie. a collection of symptoms and signs) caused by substances produced by the tumour cells which act remotely from the tumour or its metastases.

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15
Q

2 causes of paraneoplastic syndrome

A
  • it may be caused by hormones, cytokines or other factors produced by the tumour cells.
  • it may be caused by antibodies produced by the body to ‘fight’ the tumour but which unfortunately cross-react with normal tissues and damage them.
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16
Q

2 examples of paraneoplastic syndrome

A

Cushing’s syndrome

Nephrotic syndrome

17
Q

How is dysplasia characterised?

A

Dysplasia is classified (‘graded’) according to the severity of changes seen on histology:
• in some anatomical sites (eg. cervix) three grades are used: mild, moderate, severe.
• in other anatomical sites (eg. colon) two grades are used: low and high.