Prostate Cancer Flashcards

1
Q

How common is prostate cancer?

A

Prostate cancer is the most common cancer in men in the UK, accounting for 26% of all male cancer diagnoses, and is estimated that 1 in 8 men will be diagnosed with prostate cancer in their lifetime.

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2
Q

Briefly describe the pathophysiology of prostate cancer

A

Although the exact aetiology of prostate cancer is the subject of ongoing research, it is widely agreed that the growth of prostate cancer is influenced by androgens (testosterone and dihydrotestosterone (DHT)).

The majority of prostate cancers (>95%) are adenocarcinomas. Over 75% of prostate adenocarcinomas arise from the peripheral zone, with 20% in the transitional zone and 5% in the central zone. Prostate cancers are often multifocal.

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3
Q

How can prostate adenocarcinomas be classified?

A

Prostate adenocarcinomas can be categorised into two types:

  • Acinar adenocarcinoma- originates in the glandular cells that line the prostate gland
    • This is the most common form of prostate cancer
  • Ductal adenocarcinoma- originates in the cells that line the ducts of the prostate gland
    • This tends to grow and metastasise faster than acinar adenocarcinoma
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4
Q

What are the risk factors for prostate cancer?

A
  • Age
  • Ethnicity
    • Men of black African or Caribbean ethnicity are twice as likely to be diagnosed with prostate cancer in their lifetime when compared to white Caucasian men
  • Family history of prostate cancer
  • Genetic predisposition
    • BRCA2 or BRCA1 gene are at greater risk
  • Other less significant modifiable risk factors include obesity, diabetes mellitus, smoking (associated with increased risk of prostate cancer death) and degree of exercise (considered protective)
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5
Q

What are the clinical features of prostate cancer?

A

Patients can present with a wide variety of symptoms, dependent on stage of the disease. Localised disease can present with lower urinary tract symptoms (LUTS) including weak urinary stream, increased urinary frequency and urgency.

More advanced localised disease may also cause haematuria, dysuria, incontinence, haematospermia, suprapubic pain, loin pain, and even rectal tenesmus. Any metastatic disease may cause, amongst others, bone pain, lethargy, anorexia, and unexplained weight loss.

A Digital Rectal Examination (DRE) is essential if a diagnosis of prostate cancer is suspected, as most prostate adenocarcinomas arise from the posterior peripheral zone. The examination should be checking for evidence of asymmetry, nodularity, or a fixed irregular mass.

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6
Q

What is being assessed in the DRE of prostate cancer?

A

A Digital Rectal Examination (DRE) is essential if a diagnosis of prostate cancer is suspected, as most prostate adenocarcinomas arise from the posterior peripheral zone.

The examination should be checking for evidence of asymmetry, nodularity or a fixed irregular mass.

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7
Q

What is the role of Prostate Specific Antigen (PSA) in diagnosing prostate cancer?

A

Prostate Specific Antigen (PSA) is a serum protein produced by both malignant and normal healthy cells in the prostate gland. PSA can be elevated secondary to prostate cancer.

Further calculations using PSA, such as free:total PSA ratio, can be used to increase the accuracy of the test for men with PSA from 4-10; a low free:total ratio is associated with an increased chance of diagnosing prostate cancer.

PSA density can also be used, which is the serum PSA level divided by prostate volume determined by imaging (i.e. TRUS, CT, or MRI); higher PSA densities can suggest an increased likelihood of prostate cancer.

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8
Q

Give examples of other causes that can raise PSA

A

PSA can become artificially raised with several other conditions, including BPH, prostatitis, vigorous exercise, ejaculation, and recent DRE, reducing its specificity.

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9
Q

Describe the guide for normal age-adjusted serum PSA levels

A

40-49 years <2.5 ng/mL.

50-59 years <3.5 ng/mL.

60-69 years <4.5 ng/mL.

>70 years <6.5 ng/mL.

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10
Q

Is there screening for prostate cancer?

A

To date, there is no national prostate cancer screening programme in many Western countries.

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11
Q

What is the current method use to diagnose prostate cancer?

A

The current standard method for diagnosing prostate cancer is through biopsies of prostatic tissue, with two potential methods:

  • Transperineal (Template) biopsy
  • TransRectal UltraSound-guided (TRUS) biopsy
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12
Q

Briefly describe Transperineal (Template) biopsy

A

This involves sampling prostatic tissue transperineally in a systematic manner, done as a day case under general anaesthetic. The transperineal approach allows better access to the anterior part of the prostate and also has a lower risk of infection.

Shown as A on the diagram.

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13
Q

Briefly describe TransRectal UltraSound-guided (TRUS) biopsy

A

This involves sampling the prostate transrectally, usually under local anaesthetic. Generally 12 cores are taken bilaterally in equal distribution from base to apex. Transrectal biopsies are associated with a 1-2% risk of sepsis.

Shown as B on the diagram.

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14
Q

What imaging is used in prostate cancer?

A

Multi-parametric magnetic resonance imaging (mp-MRI) is increasingly used to aid in the diagnosis of prostate cancer. Mp-MRI can identify abnormal areas of the prostate, which can then be targeted for biopsy by MRI-ultrasound fusion or cognitive-guidance techniques.

Staging of prostate cancer is typically done for men with intermediate and high-risk disease. Staging is accomplished with abdomino-pelvic CT imaging and bone scan.

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15
Q

Why has mp-MRI not replaced biopsy in the diagnosis of prostate cancer?

A

Mp-MRI has not replaced biopsy in the diagnosis for prostate cancer as a subset of patients with prostate cancer will have a negative MRI.

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16
Q

What grading system is used for prostate cancer?

A

Gleason Grading System.

17
Q

Briefly describe the Gleason Grading System

A

The Gleason grading system is a scoring system by which prostate cancers are graded, based upon their histological appearance.

The sample of prostate tissue is assigned a score according to its differentiation and the Gleason Score is then calculated as the sum of the most common growth pattern + the second most common growth pattern seen.

In essence, the lowest score that can be assigned to an individual with prostate cancer is Gleason 3+3. Higher Gleason scores are associated with a poorer prognosis.

In clinical practice, Gleason scores alone are not used to determine prognosis and recurrence risk, instead the score is used in conjunction with PSA levels and TNM staging.

18
Q

What parameters are involved in risk stratification of prostate cancer?

A

Management of localised cancer relates directly to risk stratification based on PSA levels, Gleason score, and T staging (from TNM).

19
Q

What is the treatment in low-risk disease prostate cancer?

A

Most can be offered active surveillance, radical treatments offered to those who show evidence of disease progression.

20
Q

What is the treatment in intermediate and high risk disease?

A

Radical treatment options should be discussed with all men with intermediate risk disease and high risk disease with realistic disease control. Those with intermediate risk can also be offered active surveillance (should not be offered for high risk disease).

21
Q

What is the treatment in metastatic disease?

A

Chemotherapy agents and anti-hormonal agents can be used in metastatic prostate cancer.

22
Q

What is the treatment in castrate-resistant disease?

A

Those who demonstrate evidence of hormone-relapsed disease can be considered for further chemotherapy agents, such as Docetaxel. Corticosteroids can be offered as third-line hormonal therapy after androgen deprivation therapy and anti-androgen therapy to men with hormone-relapsed prostate cancer.

23
Q

When is watchful waiting commonly used?

A

Watchful waiting is generally reserved for older patients with lower life expectancy and can be offered for any stage of prostate cancer; there is no pre-define follow up protocol and management is largely guided by patient goals of care and maintaining quality of life.

24
Q

Briefly describe watchful waiting and active surveillance

A

Watchful waiting is a symptom-guided approach to prostate cancer management where definitive therapy is often deferred and hormonal therapy is initiated at time of symptomatic disease.

Active surveillance can be offered to select patients with low-risk disease and for some cases of intermediate-risk disease. Active surveillance requires monitoring of patients with 3-monthly PSA, 6 month to yearly DRE, and re-biopsy at 1-3 yearly intervals assessing for progression and intervening at the appropriate time. Mp-MRI is also being used increasingly in such protocols.

25
Q

Briefly describe the surgical management of prostate cancer

A

The mainstay surgical treatment for prostate cancer consists of a radical prostatectomy. This involves the removal of the prostate gland, resection of the seminal vesicles, along with the surrounding tissue +/- dissection of the pelvic lymph nodes.

This procedure can also be performed with an open approach, laparoscopically or robotically.

26
Q

What are the side effects of radical prostectomy?

A

Side effects of radical prostatectomy include erectile dysfunction (affecting 60-90% of men), stress incontinence and bladder neck stenosis.

27
Q

Briefly describe the use of radiotherapy of prostate cancer

A

External-beam radiotherapy and brachytherapy are both commonly used alternatives as a form of curative intervention for localised prostate cancer.

Brachytherapy involves the transperineal implantation of radioactive seeds (usually Iodine-125) directly into the prostate gland.

External-beam radiotherapy uses focused radiotherapy to target the prostate gland and limiting damage to surrounding tissues.

28
Q

Briefly describe the use of chemotherapy for prostate cancer

A

Chemotherapy is usually only indicated in patients with metastatic prostate cancer.

Some examples of chemotherapy drugs used include docetaxel (recommended in men with testosterone-resistant cancer) and cabazitaxel (used with prednisolone, recommended for treating relapsed prostate cancer which has progressed after using docetaxel chemotherapy).

29
Q

Briefly describe the use of anti-androgen therapy in prostate cancer

A

As prostate cancer growth is stimulated by circulating androgens (testosterone), androgen deprivation therapies are regularly used, such as via gonadotrophin-releasing hormone (GnRH) receptor agonists (e.g. goserelin)

Newer hormone therapies now exist, such as the drugs enzalutamide and abiraterone, acting to lower levels of serum testosterone. Both of these drugs are reserved for patients with metastatic prostate cancer.

30
Q

What differentials should be considered for prostate cancer?

A
  • Benign prostatic hyperplasia (BPH)
  • Prostatitis
  • Other causes of haematuria: these may include bladder cancer, urinary stones, urinary tract infections and pyelonephritis
31
Q

How does BPH and prostate cancer differ?

A

A non-cancerous enlargement of the prostate gland, will also cause LUTS symptoms initially.

32
Q

How does prostatitis and prostate cancer differ?

A

Inflammation of the prostate gland. Patients usually present with perineal pain, with neutrophils seen on urinalysis.