Cancer diagnosis: is it a tumour?

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Cancer Biology Mind Map on Cancer diagnosis: is it a tumour?, created by maisie_oj on 09/04/2013.
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Mind Map by maisie_oj, updated more than 1 year ago
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Created by maisie_oj over 11 years ago
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Cancer diagnosis: is it a tumour?
  1. Screening
    1. ... In the UK
      1. Only done when... (criterea)
        1. Condition is an important health problem, well understood disease, recognisable at an early stage treatment is more effective at early stages...
          1. Suitable/acceptable tests exist, facilities exist to cope with abnormalitites detected...
            1. Resources exist to allow for multiple/repeated screens at age of risk and the harms and costs are outweighed by the benefits
        2. Screens
          1. Cervical
            1. Well defined disease progression (Normal, CIN I, CIN II and CIN III)
              1. Women aged 25-6yrs
                1. 25-49yrs (highest risk) = every 3yrs
                  1. 50-64yrs (lower risk) = every 5yrs
                    1. >65yrs - not screened unless they havn't been screened since 50yrs or abnormal smear seen
                      1. If 80% of the population screened then there would be a 95%reduction in the death rate from cervical cancer
                        1. "Jade Goody" effect
                          1. 33,000 more smears than expected, 35% during the month of her death
                            1. The biggest increase seen in 25-29yrs age range
                              1. Now this surge in women being screened is already trailing off
                            2. A negative screen can provide 41-69% protection in women aged 20-54yrs and 73% protection in >55yrs
                              1. ... with 3-yearly intervals between screens
                                1. Protection drops with 5-yearly intervals
                          2. Two techniques...
                            1. (Classical) 'Pap' smear
                              1. Spatula scrapes cells from the surface of the cervix
                                1. Must ensure to swab the 'transition zone' (where most neoplasms occur)
                                  1. = the border between the stratified squamous epithelium of the cervix and the columnar mucous epithelium of the vagina
                                    1. Swab spread onto glass slide and observed (microscopy)
                                2. (Newer) Liquid-based cytology
                                  1. Same swab taken as in the 'pap' smear
                                    1. Swab tip is broken off into a solution of preservative
                                      1. This is spun to remove debris and other obstructive material (mucous etc.)
                                        1. Automated machine removes the cells and spreads a thin layer onto a glass slide
                                          1. Slide observed under microscope
                                3. HPV and cervical cancer
                                  1. Epidemiological studies indicate cervical cancer as an STD
                                    1. HPV found in 85% of cervical carcinomas
                                    2. High risk forms (= 16, 18, 31, 33, 35, 55 - found in ~100% of invasive cervical carcinomas) and low risk forms (= 6 and 11 - cause genital warts only)
                                      1. HPV also involved in; anus, penile, vulval, throat and mouth cancers too
                                      2. Pathogenesis and carcinogenesis
                                        1. Sexual contact -> HPV exposure
                                          1. Cervical transmformation zone (infection)
                                            1. Integration of viral DNA into host DNA
                                              1. HPV proteins E6 (inhibits p53) and E7 (inhibits; p53, p21 and Rb) - cause avoidance of apoptosis and premature entry into S-phase
                                                1. Squamous / endocervical columnar differentiation
                                                  1. High/low grade squamous intraepithelial lesions / glandular intraepithelial lesions
                                                    1. Carcinogenic risk factors; smoking, oral contraceptives, high parity (given birth many times), altered immune status, gene mutations, time
                                                      1. Invasive; squamous carcinoma / adenocarcinoma
                                            2. 75% of population exposed to HPV (only 50% to high risk HPV)
                                              1. of these - 10% have persistent CIN (cervical intraepithelial neoplaisa)
                                                1. 1.3% progress to invasive carcinoma
                                                  1. 0.4% die
                                          2. HPV vaccination
                                            1. Started in (sept) 2008; offered to all 12-13 and 17-18yo females
                                              1. x3 injections over 6 (or 12) months
                                                1. Two vaccines
                                                  1. Cervarix (protects against HPV 16 and 18)
                                                    1. Gardasil (protects against HPV 6 AND 11)
                                                      1. Unanswered questions
                                                        1. How long does protection last?
                                                          1. Is there cross-protection (from other serotypes)?
                                                            1. Will other types of HPV become carcinogenic?
                                                    2. In US 62.5% of males are HPV positive
                                                      1. Need to vaccinate boys?
                                                  2. High risk HPV found in ~100% of invasive cervical carcinomas
                                                    1. Screen for these HPV's by PCR?
                                                  3. Breast
                                                    1. Based on mammography - aimed at detecting calcification
                                                      1. Calcification associated with ductal carcinoma in situ (DCIS)
                                                        1. Pre-invasive
                                                          1. No metastatic capacity
                                                            1. Curable
                                                          2. NHS breast screening programme (BSP): invites women 50-70yrs (highest risk)
                                                            1. screened every 3 years
                                                              1. Is this too long?
                                                              2. Saves 1400 lives per year in England
                                                                1. Is 50yrs the right age?
                                                                  1. Now inviting women at 47yrs
                                                                  2. Is this screening necessary?
                                                                    1. BBC health news - reports a third of breast cancer as being 'harmless'
                                                                      1. An independent review, published in the Lancet (2012) - highlights the problem of overdiagnosing cancer
                                                                        1. This is the detection of a cancer that would not otherwise cause that person a problem during their lifetime
                                                                          1. Waste of time/resources?
                                                                            1. Unecessary treatment and follow up to the individual?
                                                                              1. Further screening, biopsies - unecessary pain/stress?
                                                                          2. The future of breast screening
                                                                            1. It is unlikely that breast cancer screening will stop
                                                                              1. Instead aim is to target high risk individuals - family history / high mammographic density
                                                                                1. Clinical trial in discussion: 'watch and wait' method for DCIS
                                                                            2. Once imaging done - biopsy
                                                                              1. Fine needle aspirate (sample fluid around mass)
                                                                                1. Core needle (removes a 'core' of mass)
                                                                                  1. Vaccum (removes a larger sample of mass)
                                                                                    1. Large core biopsy (larger core - may also remove healthy tissue)
                                                                                      1. Surigical (entire mass cut out under anaesthetics)
                                                                                    2. Bowel
                                                                                      1. 1 in 20 people develop colorectal cancer (3rd most common cancer in UK and 2nd leading cause of death (after lung))
                                                                                        1. Screening aimed at detecting the non-malignant polyps (adenomas) - usually present early as blood in stool
                                                                                          1. Based on faecal occult blood (FOB) testing
                                                                                            1. Who?: men and women 50-69yrs
                                                                                              1. When?: every 2yrs
                                                                                                1. Results: 98% have normal result
                                                                                                  1. 2% have positive FOB
                                                                                                    1. Invited for colonoscopy
                                                                                                      1. 50% of these - normal
                                                                                                        1. 40% of these - adenoma
                                                                                                          1. 10% of these - carcinoma (mostly early stage)
                                                                                                            1. Risk: 1/1500 chance in bowel perforation
                                                                                                    2. Currently no screen for...
                                                                                                      1. Ovarian
                                                                                                        1. In 2008... 6,500 cases; 4,400 deaths
                                                                                                          1. 5th most common cancer in women (lifetime risk = 1 in 54)
                                                                                                            1. Accounts for 6% of deaths from cancer in women (more then any other gynae cancer in women)
                                                                                                            2. No current test specific enough
                                                                                                              1. Two tests being trialled
                                                                                                                1. CA125
                                                                                                                  1. Circulating tumour marker
                                                                                                                    1. Raised in 85% of ovarian cancer cases
                                                                                                                      1. Raised in 50% in early stages of ovarian cancer
                                                                                                                        1. Other causes can raise this marker
                                                                                                                        2. Trans-vaginal ultrasound
                                                                                                                          1. Ultrasound probe is inserted into the vagina and imaging of the deeper reproductive organs possible through the vaginal wall
                                                                                                                          2. Being used in a screening trial (UKCTOCS - UK collaborative trial of ovarian cancer screening)
                                                                                                                            1. Screening of general female population 50-74yrs
                                                                                                                              1. Women selected at random from GP lists and invited
                                                                                                                                1. To date 10,000 post-menopausal women screened
                                                                                                                                  1. Detected 58 cancers
                                                                                                                                    1. Missed 12 cancers (6 of these were early stage)
                                                                                                                                  2. Group 1 - annual CA125 measure if abnormal U/S
                                                                                                                                    1. Group 2 - annual U/S, if abnormal CA125
                                                                                                                                      1. Group 3 - No screening
                                                                                                                              2. Prostate
                                                                                                                                1. No screening programme - but a risk management programme
                                                                                                                                  1. Based on advice to take up Prostate-specific antigen (PSA) testing
                                                                                                                                    1. PSA gives a lot of false negatives
                                                                                                                                      1. 10% of all men 50-65yrs will have raised PSA
                                                                                                                                        1. Only 25% of these will have prostate cancer
                                                                                                                                          1. Next step: trans-rectal ultrasound (U/S) and biopsyn under prophylactic antibiotics
                                                                                                                                            1. Positive result: treatment is by radical prostatectomy or radical radiotherapy
                                                                                                                                              1. Prostate cancer is highly hetergenous (differs massively between individual)
                                                                                                                                                1. Therefore no evidence that early treatment improves survival
                                                                                                                                                  1. More men die with - rather than from - prostate cancer
                                                                                                                                2. Other screening techniques?
                                                                                                                                  1. Microarrays
                                                                                                                                    1. Gavaert, 2009
                                                                                                                                      1. Used microarrays to identify gene clusters associated with tissue specific primary tumours and their metastases
                                                                                                                                        1. Recognised; breast, colon, lung, ovarian, prostate, kidney and thyroid/kidney clusters of gene expression in epithelial cancers
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