Early prostate cancer usually causes no symptoms. As a tumor grows beyond the prostate, it can damage nearby organs causing erectile dysfunction, blood in the urine or semen, or trouble urinating – often frequent urination and slow or weak urine stream.^[4] More than half of men over age 50 experience some form of urination problem,^[5] typically due to issues other than prostate cancer such as benign prostatic hyperplasia (non-cancerous enlargement of the prostate).^[4]

Advanced prostate tumors often metastasize to nearby bones of the pelvis and back; there they can cause fatigue, unexplained weight loss, and back or bone pain that does not improve with rest.^[6] Metastases can damage the bones around them, and around a quarter of those with metastatic prostate cancer develop a bone fracture.^[7] Growing metastases can also compress the spinal cord causing weakness in the legs and feet, or limb paralysis.^[8][9]

Most cases of prostate cancer are diagnosed through screening tests, when tumors are too small to cause any symptoms.^[4] This is done through blood tests to measure levels of the protein prostate-specific antigen (PSA), which are elevated in those with enlarged prostates, whether due to prostate cancer or benign prostatic hyperplasia.^[10][11] The average man's blood has around 1 nanogram (ng) of PSA per milliliter (mL) of blood tested.^[12] Those with PSA levels below average are very unlikely to develop dangerous prostate cancer over the next 8 to 10 years.^[12] Men with PSA levels above 4 ng/mL are at increased risk – around 1 in 4 will develop prostate cancer – and are often referred for a prostate biopsy.^[13][14] PSA levels over 10 ng/mL indicate higher risk still; over half of men in this group develop prostate cancer.^[13] Men with high PSA levels are often recommended to repeat the blood test four to six weeks later, as PSA levels can fluctuate unrelated to prostate cancer.^[15]

Those with elevated PSA may undergo secondary screening blood tests that measure subtypes of PSA and other molecules to better predict the likelihood that a person will develop aggressive prostate cancer. In particular, many measure "free PSA" – the around 10–30% of PSA unbound to other blood proteins. Men who have a lower percentage of free PSA are more likely to have prostate cancer.^[16] Several common tests more accurately detect prostate cancer cases by also measuring subtypes of free PSA, including the Prostate Health Index (measures a fragment called -2proPSA) and 4K score (measures intact free PSA).^[17][18] Other tests measure blood levels of additional prostate-related proteins such as kallikrein-2 (also measured by 4K score), or urine levels of mRNA molecules common to prostate tumors like PCA3 and TMPRSS2 fused to ERG.^[19]

Several large studies have found that men screened for prostate cancer have a reduced risk of dying from the disease;^[20] however, detection of cancer cases that would not have otherwise impacted health can cause anxiety, and lead to unneeded biopsies and treatments.^[10] Major national health organizations offer differing recommendations, attempting to balance the benefits of early diagnosis with the potential harms of treating people whose tumors are unlikely to impact health.^[10] Most medical guidelines recommend that men in good health and at high risk of prostate cancer (due to age, family history, ethnicity, or prior evidence of high blood PSA levels) be counseled on the risks and benefits of PSA testing, and be offered access to screening tests.^[10] Uptake of screening varies by geography – more than 80% of men are screened in the US and Western Europe, 20% of men in Japan, and screening is rare in regions with a low Human Development Index.^[20]

Men suspected of having prostate cancer may undergo several tests to help assess the prostate. One common procedure is the digital rectal examination, in which a doctor inserts a lubricated finger into the rectum to feel the nearby prostate.^[21][22] Tumors feel like stiff, irregularly shaped lumps against the rest of the prostate. Hardening of the prostate can also be due to benign prostatic hyperplasia; around 20–25% of those with abnormal findings on their rectal exams have prostate cancer.^[23]

A diagnosis of prostate cancer requires a biopsy of the prostate. Prostate biopsies are typically taken by a needle passing through the rectum or perineum, guided by transrectal ultrasound imaging, magnetic resonance imaging (MRI), or a combination of the two.^[24][22] Ten to twelve samples are taken from several regions of the prostate to improve the chances of finding any tumors.^[22] Biopsies are examined under a microscope by a pathologist, who determines the type and extent of cancerous cells present. Cancers are first classified based on their appearance under a microscope. Over 95% of prostate cancers are classified as adenocarcinomas (resembling gland tissue), with the rest largely squamous-cell carcinoma (resembling squamous cells, a type of epithelial cell) and transitional cell carcinoma (resembling transitional cells).^[25]

Next tumor samples are graded based on how much the tumor tissue differs from normal prostate tissue; the more different the tumor appears, the faster the tumor is likely to grow. The Gleason grading system is commonly used, where the pathologist assigns a number from 1 (most similar to healthy prostate tissue) to 5 (least similar) for the most common pattern observed under the microscope, then does the same for the second-most common pattern. The sum of these two numbers is the Gleason score.^[25] The total scores of 2 through 5 are no longer commonly used in practice, making the lowest score 6, and the highest score 10. Scores are commonly grouped into Gleason grade groups: a score of 6 or lower is Gleason grade group 1; a score of 7 with the first number (from the most common pattern) 3 and the second number 4 is grade group 2; the reverse – first number 4, second number 3 – is grade group 3; a score of 8 is grade group 4; a score of 9 or 10 is grade group 5.^[25] Higher Gleason scores and higher grade groups represent cancer cases likely to be more aggressive with a worse prognosis.^[25]

The extent of cancer spread is assessed by MRI or PSMA scan – a positron emission tomography (PET) imaging technique where a radioactive label that binds the prostate protein prostate-specific membrane antigen is used to detect metastases distant from the prostate.^[26][22] CT scans may also be used, but are less able to detect spread outside the prostate than MRI. Bone scintigraphy is used to test for spread of cancer to bones.^[26]

Staging edit

After diagnosis, the tumor is staged to determine the extent of its growth and spread. Prostate cancer is typically staged using the American Joint Committee on Cancer's (AJCC) three-component TNM system, with scores assigned for the extent of the tumor (T), spread to any lymph nodes (N), and the presence of metastases (M).^[27] Scores of T1 and T2 represent tumors that remain within the prostate: T1 is for tumors not detectable by imaging or digital rectal exam; T2 is for tumors detectable by imaging or rectal exam, but still confined within the prostate.^[28] T3 is for tumors that grow beyond the prostate – T3a for tumors with any extension outside the prostate; T3b for tumors that invade the adjacent seminal vesicles. T4 is for tumors that have grown into organs beyond the seminal vesicles.^[28] The N and M scores are binary (yes or no). N1 represents any spread to the nearby lymph nodes. M1 represents any metastases to other body sites.^[28]

The AJCC then combines the TNM scores, Gleason grade group, and results of the PSA blood test to categorize cancer cases into one of four stages, and their subdivisions. Cancer cases with localized tumors (T1 or T2), no spread (N0 and M0), Gleason grade group 1, and PSA less than 10 ng/mL are designated stage I. Those with localized tumors and PSA between 10 and 20 ng/mL are designated stage II – subdivided into IIA for Gleason grade group 1, IIB for grade group 2, and IIC for grade group 3 or 4. Stage III is the designation for any of three higher risk factors: IIIA is for a PSA level about 20 ng/mL; IIIB is for T3 or T4 tumors; IIIC is for a Gleason grade group of 5. Stage IV is for cancers that have spread to lymph nodes (N1, stage IVA) or other organs (M1, stage IVB).^[27]

The United Kingdom National Institute for Health and Care Excellence recommends a five-stage system based on disease prognosis called the Cambridge Prognostic Group, with prognostic groups CPG 1 to CPG 5.^[29] CPG 1 is the same as AJCC stage I. Cases with localized tumors (T1 or T2) and either Gleason grade group 2 or higher PSA levels (10 to 20 ng/mL) are designated CPG 2. CPG 3 represents either Gleason grade group 3, or the combination of the CPG 2 criteria. CPG 4 is similar to AJCC stage 3 – any of Gleason grade group 4, PSA levels above 20 ng/mL, or a tumor that has grown beyond the prostate (T3). CPG 5 is for the highest risk cases: either a T4 tumor, Gleason grade group 5, or any two of the CPG 4 criteria.^[30]

No drug or vaccine is approved by regulatory agencies for the prevention of prostate cancer. Several studies have shown 5α-reductase inhibitors to reduce the total incidence of prostate cancer; however, it remains unclear whether they reduce any cases of dangerous disease.^[31]

Treatment of prostate cancer varies based on how advanced the cancer is, the risk it may spread, and the affected person's health and personal preferences.^[32] Those with localized disease at low risk for spread are often more likely to be harmed by the side effects of treatment than the disease itself, and so are monitored regularly by repeat testing for a worsening of their disease.^[33] Those at higher risk may receive treatment to eliminate the tumor – typically prostatectomy (surgery to remove the prostate) or radiation therapy, sometimes alongside hormone therapy.^[34] Those with metastatic disease are additionally treated with chemotherapy, as well as additional radiation or other agents to alleviate the symptoms of metastatic tumors.^[34] Throughout the treatment course, blood PSA levels are monitored to assess the effectiveness of treatments, and whether the disease is advancing.^[35]

Localized disease edit

Men diagnosed with low-risk cases of prostate cancer often defer treatment and are monitored regularly for cancer progression by active surveillance, which involves monitoring the tumor for growth at fixed intervals by PSA tests (around every six months), digital rectal exam (annually), and MRI or repeat biopsies (every one to three years).^[33] This program continues until increases in PSA levels, Gleason grade, or tumor size indicate a higher-risk tumor that may require intervention.^[36] At least half of men remain on active surveillance, never requiring more direct treatment for their prostate tumors.^[37]

Those who elect to have therapy typically receive radiation therapy or a prostatectomy.^[38] Radiation can be delivered by intensity-modulated radiation therapy (IMRT), which allows for high doses (greater than 80 Gy) to be delivered to the prostate with relatively little radiation to other organs, or by brachytherapy, where a radioactive source is surgically placed next to the prostate.^[39][40] IMRT is given over several sessions, with treatments repeated five days per week for several weeks. Brachytherapy is typically performed in a single session, with the radioactive source permanently implanted into the prostate, where it expends its radioactivity within the next few months.^[41] With either technique, radiation damage to nearby organs can increase the risk of subsequent bladder cancer and cause erectile dysfunction, infertility, and gastrointestinal problems: diarrhea, bloody stools, fecal incontinence, and pain.^[42]

Radical prostatectomy aims to surgically remove the cancerous part of the prostate, along with the seminal vesicles, and parts of the vas deferens.^[43] This is typically done by robot-assisted surgery, where robotic tools inserted through small holes in the abdomen allow a surgeon to make small and exact movements during surgery.^[44] This method results in shorter hospital stays, less blood loss, and fewer complications than traditional open surgery.^[44] In places where robot-assisted surgery is unavailable, prostatectomy can be performed laparoscopically (using a camera and hand tools through small holes in the abdomen), or through traditional open surgery with an incision above the penis (retropubic approach) or below the scrotum (perineal approach).^[45][44] The four approaches result in similar rates of cancer control.^[45] Damage to nearby tissue during surgery can result in erectile dysfunction and urinary incontinence. Erectile dysfunction is more likely in those who are older or had previous erectile issues.^[45] Incontinence is more common in those who are older and have shorter urethras.^[45] Both for cancer progression outcomes and surgical side effects, the skill and experience of the individual surgeon doing the procedure are among the greatest determinants of success.^[45]

Radiotherapy and surgery result in similar outcomes with respect to bowel, erectile and urinary function after five years.^[46] After prostatectomy, PSA levels drop rapidly, reaching very low or undetectable levels within two months. Radiotherapy also substantially reduces PSA levels, but more slowly and less completely, with PSA levels reaching their nadir two years after radiotherapy.^[47] After either treatment, PSA levels are monitored regularly. Up to half of those treated will eventually have a rise in PSA levels, suggesting the tumor or small metastases are growing again.^[48] People with high or rising PSA levels are often offered another round of radiation therapy directed at the former tumor site. This reduces risk for further progression by 75%.^[49] Those suspected of metastases can undergo PET scanning with sensitive radiotracers C-11 choline, F-18 fluciclovine, and F-18 or Ga-68 attached to a PSMA-targeting drug, each of which is able to detect small metastases more sensitively than alternative imaging methods.^[50][49]

Metastatic disease edit

For those with metastatic disease, the standard of care is androgen deprivation therapy, drugs that reduce levels of androgens (male sex hormones) that prostate cells require to grow.^[51] Various drugs are used to lower androgen levels by blocking the synthesis or action of testosterone, the primary androgen. The first line of treatment is typically GnRH agonists like leuprolide, goserelin, or triptorelin by injection monthly or less frequently if needed.^[52][51] GnRH agonists cause a brief rise in testosterone levels at treatment initiation, which can worsen disease in people with significant symptoms of metastases.^[53] In these people, GnRH antagonists like degarelix or relugolix are given instead, and can also rapidly reduce testosterone levels.^[53] Hormone therapy halts tumor growth in more than 95% of those treated,^[54] and PSA levels return to normal in up to 70%.^[55]

Despite reduced testosterone levels, metastatic prostate tumors eventually continue to grow – manifested by rising blood PSA levels, and metastases to nearby bones.^[56][57] This is the most advanced stage of the disease, called castration-resistant prostate cancer (CRPC). CRPC tumors continuously evolve resistance to treatments, necessitating several lines of therapy, each used in sequence to extend survival. The standard of care is the chemotherapy docetaxel along with antiandrogen drugs, namely the androgen receptor antagonists enzalutamide, apalutamide, and darolutamide, as well as the testosterone production inhibitor abiraterone acetate.^[58][56][59] An alternative is the cell therapy procedure Sipuleucel-T, where the affected person's immune cells are removed, treated to more effectively target prostate cancer cells, and re-injected into the same person.^[56] Tumors that evolve resistance to docetaxel may receive the second-generation taxane drug cabazitaxel.^[56]

Some CRPC treatments are used only in men whose tumors have certain characteristics that make the therapy more likely to be effective. Men whose tumors express the protein PSMA may receive the radiopharmaceutical Lu-177 PSMA, which binds to and destroys PSMA-positive cells.^[60][56] Those whose tumors have defective DNA damage repair benefit from treatment with the immune checkpoint inhibitor drug pembrolizumab and/or PARP inhibitors, namely olaparib, rucaparib, or niraparib.^[56]

Supportive care edit

Bone metastases – present in around 85% of those with metastatic prostate cancer – are the primary cause of symptoms and death from metastatic prostate cancer.^[61][62] Those with constant pain are prescribed nonsteroidal anti-inflammatory drugs.^[63] However, people with bone metastases often experience "breakthrough pain", sudden bursts of severe pain that resolve within around 15 minutes, before pain medications can take effect.^[63] Single sites of pain can be treated with external beam radiation therapy to shrink nearby tumors.^[64] More dispersed bone pain can be treated with radioactive compounds that disproportionately accumulate in bone, like radium-223 and samarium-153-EDTMP, which help reduce the size of bone tumors. Similarly, the systemic chemotherapeutics used for metastatic prostate cancer can reduce pain as they shrink tumors.^[64] Other bone modifying agents like zoledronic acid and denosumab can reduce prostate cancer bone pain, even though they have little effect on tumor size.^[64] Metastases compress the spinal cord in up to 12% of those with metastatic prostate cancer causing pain, weakness, numbness, and paralysis.^[65][66] Inflammation in the spine can be treated with high-dose steroids, as well as surgery and radiotherapy to shrink spinal tumors and relieve pressure on the spinal cord.^[65][66]

Those with advanced prostate cancer often suffer fatigue, lethargy, and a generalized weakness. This is caused in part by gastrointestinal problems, with loss of appetite, weight loss, nausea, and constipation all common. These are typically treated with appetite-increasing drugs – megestrol acetate or corticosteroids – antiemetics, or treatments that focus on underlying gastrointestinal issues.^[67] General weakness can also be caused by anemia, itself caused by a combination of the disease itself, poor nutrition, and damage to the bone marrow from cancer treatments or bone metastases.^[68] Anemia can be treated in various ways depending on the cause, or can be addressed directly with blood transfusions.^[68] Organ damage and metastases in the lymph nodes can lead to uncomfortable accumulation of fluid (called lymphedema) in the genitals or lower limbs. These swellings can be extremely painful, curtailing an affected person's ability to urinate, have sex, or walk normally. Lymphedema can be treated by applying pressure to aid drainage, surgically draining pooled fluid, and cleaning and treating nearby damaged skin.^[69]

People with prostate cancer are around twice as likely to experience anxiety or depression compared to those without cancer.^[70] When added to normal prostate cancer treatments, psychological interventions such as psychoeducation and cognitive behavioral therapy can help reduce anxiety, depression, and general distress.^[71]

As those severely ill with metastatic prostate cancer near the end of their lives, most experience confusion and may hallucinate or have trouble recognizing loved ones.^[72][73] Confusion is caused by various conditions, including kidney failure, sepsis, dehydration, and as a side effect of various drugs, especially opioids.^[72] Most people sleep for long periods, and some feel drowsy when awake.^[73] Restlessness is also common, sometimes caused by physical discomfort from constipation or urinary retention, sometimes caused by anxiety.^[73] In their last few days, affected men's breathing may become shallow and slow, with long pauses between breaths. Breathing may be accompanied by a rattling noise as fluid lingers in the throat, but this is not uncomfortable for the affected person.^[73][74] Their hands and feet may cool to the touch, and skin become blotchy or blue due to weaker blood circulation. Many stop eating and drinking, resulting in dry-feeling mouth, which can be aided by moistening the mouth and lips.^[73] The person becomes less and less responsive, and eventually the heart and breathing stop.^[74]

The prognosis of diagnosed prostate cancer varies widely based on the cancer's grade and stage at the time of diagnosis; those with lower stage disease have vastly improved prognoses. Around 80% of prostate cancer diagnoses are in men whose cancer is still confined to the prostate. These men often survive long after diagnosis, with as many as 99% still alive 10 years from diagnosis.^[75] Men whose cancer has metastasized to a nearby part of the body (around 15% of diagnoses) have poorer prognoses, with five-year survival rates of 60–80%.^[76] Those with metastases in distant body sites (around 5% of diagnoses) have relatively poor prognoses, with five-year survival rates of 30–40%.^[76]

Those who have low blood PSA levels at diagnosis, and whose tumors have a low Gleason grade and less-advanced clinical stage tend to have better prognoses.^[77] After prostatectomy or radiotherapy, those who have a short time between treatment and a subsequent rise in PSA levels, or a rapid rate of PSA level increases are more likely to die from their cancers.^[48] Castration-resistant metastatic prostate cancer is incurable,^[78] and kills a majority of those whose disease reaches this stage.^[56]

Prostate cancer is caused by the accumulation of genetic mutations to the DNA of cells in the prostate. These mutations affect genes involved in cell growth, replication, cell death, and DNA damage repair.^[79] Changes to these genes can cause cells in the prostate to grow uncontrollably, resulting in a tumor.^[80] Over time, the tumor may grow large enough to invade nearby organs such as the seminal vesicles or bladder.^[81] Eventually, tumor cells develop the ability to travel through the lymphatic system to nearby lymph nodes, or through the bloodstream to the bone marrow and (more rarely) other body sites.^[82] At these new sites, the cancer cells disrupt normal body function and continue to grow. Metastases cause most of the discomfort associated with prostate cancer, and eventually can kill the affected person.^[82]

Most prostate tumors begin in the peripheral zone – the outermost part of the prostate.^[83] As cells begin to grow out of control, they form a small clump of disregulated cells called a prostatic intraepithelial neoplasia (PIN).^[84] Some PINs continue to grow, forming layers of tissue that stop expressing genes common to their original tissue location – p63, cytokeratin 5, and cytokeratin 14 – and begin expressing genes common to cells that makeup the innermost lining of the pancreatic duct – cytokeratin 8 and cytokeratin 18.^[83] These multilayered PINs also often overexpress the gene AMACR, which is associated with prostate cancer progression.^[83]

Particularly large PINs can eventually grow into tumors. This is commonly accompanied by large-scale changes to the genome, with chromosome sequences being rearranged or copied repeatedly. Some genomic alterations are particularly common in early prostate cancer, namely gene fusion between TMPRSS2 and the oncogene ERG (up to 60% of prostate tumors), mutations that disable SPOP (up to 15% of tumors), and mutations that hyperactivate FOXA1 (up to 5% of tumors).^[83]

Metastatic prostate cancer tends to have more genetic mutations than localized disease.^[85] Many of these mutations are in genes that protect from DNA damage, such as p53 (mutated in 8% of localized tumors, more than 27% of metastatic ones) and RB1 (1% of localized tumors, more than 5% of metastatic ones).^[85] Similarly mutations in the DNA repair-related genes BRCA2 and ATM are rare in localized disease but found in at least 7% and 5% of metastatic disease cases respectively.^[85]

The transition from castrate-sensitive to castrate-resistant prostate cancer is also accompanied by the acquisition of various gene mutations. In castrate-resistant disease, more than 70% of tumors have mutations in the androgen receptor signaling pathway – amplifications and gain-of-function mutations in the receptor gene itself, amplification of its activators (e.g. FOXA1), or inactivating mutations in its negative regulators (e.g. ZBTB16 and NCOR1).^[85] These androgen receptor disruptions are only found in up to 6% of biopsies of castrate-sensitive metastatic disease.^[85] Similarly, deletions of the tumor suppressor PTEN are harbored by 12–17% of castrate-sensitive tumors, but over 40% of castrate-resistant tumors.^[85] Less commonly, tumors have aberrant activation of the Wnt signaling pathway via disruption of members APC (9% of tumors) or CTNNB1 (4% of tumors); or dysregulation of the PI3K pathway via PI3KCA/PI3KCB mutations (6% of tumors) or AKT1 (2% of tumors).^[85]

Prostate cancer is the second-most frequently diagnosed cancer in men, and the second-most frequent cause of cancer death in men (after lung cancer).^[2][3] Around 1.2 million new cases of prostate cancer are diagnosed each year, and 350,000 men die of the disease.^[2] One in eight men are diagnosed with prostate cancer in their lifetime, and around one in forty die of the disease.^[3] Rates of prostate cancer rise with age. Due to this, prostate cancer rates are generally higher in parts of the world with higher life expectancy, which also tend to be areas with higher gross domestic product and higher human development index.^[2] Australia, Europe, North America, New Zealand, and parts of South America have the highest incidence. South Asia, Central Asia, and sub-Saharan Africa have the lowest incidence of prostate cancer; though incidence is increasing in these regions at among the fastest rates in the world.^[2] Prostate cancer is the most diagnosed cancer in men in over half of the world's countries, and the leading cause of cancer death in men in around a quarter of countries.^[86]

Prostate cancer is rare in those under 40 years old,^[87] and most cases occur in those over 60 years,^[2] with the average person diagnosed at 67.^[88] The average person who dies from prostate cancer is 77.^[88] Only a minority of prostate cancer cases are ever diagnosed. Autopsies of men who died at various ages have shown cancer in the prostates of over 40% of men over age 50. Incidence rises with age, and nearly 70% of men autopsied at age 80–89 had cancer in their prostates.^[89]

Genetics edit

Prostate cancer is more common in some families. Men with an affected first-degree relative (father or brother) have more than twice the risk of developing prostate cancer, and those with two first-degree relatives have a five-fold greater risk compared with men with no family history.^[90] Increased risk also runs in some ethnic groups, with men of African and African-Caribbean ancestry at particularly high risk – having prostate cancer at higher rates, and having more-aggressive prostate cancers that develop at earlier ages.^[91] Large genome-wide association studies have identified over 100 gene variants associated with increased prostate cancer risk.^[92] The greatest risk increase is associated with variations in BRCA2 (up to an eight-fold increased risk) and HOXB13 (three-fold increased risk), both of which are involved in repairing DNA damage.^[92] Variants in other genes involved in DNA damage repair have also been associated with an increased risk of developing prostate cancer – particularly early-onset prostate cancer – including BRCA1, ATM, NBS1, MSH2, MSH6, PMS2, CHEK2, RAD51D, and PALB2.^[92] Additionally, variants in the genome near the oncogene MYC are associated with increased risk.^[92] As are single-nucleotide polymorphisms in the vitamin D receptor common in African-Americans, and in the androgen receptor, CYP3A4, and CYP17 involved in testosterone synthesis and signaling.^[90] Together known gene variants are estimated to cause around 25% of prostate cancer cases, including 40% of early-onset prostate cancers.^[90]

Body and lifestyle edit

Men who are taller are at a slightly increased risk for developing prostate cancer, as are men who are obese.^[93] High levels of blood cholesterol are also associated with increased prostate cancer risk; consequently, those who take the cholesterol-lowering drugs, statins, have a reduced risk of advanced prostate cancer.^[94] Chronic inflammation can cause various cancers. Potential links between infection (or other sources of inflammation) and prostate cancer have been studied but none definitively found, and one large study found no link between prostate cancer and a history of gonorrhea, syphilis, chlamydia, or infection with various human papillomaviruses.^[95]

Regular vigorous exercise may reduce one's chance of developing advanced prostate cancer, as can several dietary interventions.^[96] Those with a diet rich in cruciferous vegetables, fish, genistein, or lycopene (found in tomatoes) are at a reduced risk of symptomatic prostate cancer.^[90][97] Conversely, those who consume high levels of dietary fats, polycyclic aromatic hydrocarbons (from cooking red meats), or calcium may be at an increased risk of developing advanced prostate cancer.^[90][98] Several dietary supplements have been studied and found not to impact prostate cancer risk, including selenium, vitamin C, vitamin D, and vitamin E.^[31][98]

A tumor in the prostate was first described in 1817 by the English surgeon George Langstaff, following the autopsy of a man who had died at age 68 with lower-body pain and urinary issues.^[99][100] In 1853, London Hospital surgeon John Adams described another prostate tumor from a man who had died with urinary issues; Adams had a pathologist examine the tumor, providing the first histologically confirmed case of a cancerous tumor in the prostate.^[99][101] The disease was initially thought to be uncommon as it was rarely distinguished from other causes of urinary obstruction.^[102] An 1893 report found only 50 cases described in the medical literature.^[103] Around the turn of the 19th century, prostate surgery to relieve urinary obstruction became more common, allowing surgeons and pathologists to examine the removed prostate tissue. Two studies around the time found cancer in as many as 10% of surgical specimens, suggesting prostate cancer was a fairly common cause of prostate enlargement.^[103]

For much of the 20th century, the primary therapy for prostate cancer was surgery to remove the prostate. Perineal prostatectomy was first performed in 1904 by Hugh H. Young at Johns Hopkins Hospital.^[104][105] Young's method became the widespread standard, initially done primarily to relieve symptoms of urinary blockage.^[104] In 1931 a new surgical method, transurethral resection of the prostate, became available, replacing perineal prostatectomy for symptomatic relief of obstruction.^[103] In 1945, Terence Millin described a retropubic prostatectomy approach, which provided easier access to pelvic lymph nodes to assist in staging the extent of disease, and was easier for surgeons to learn.^[104] This was improved upon by Patrick C. Walsh's 1983 description of a retropubic prostatectomy approach that avoided damage to the nerves near the prostate, preserving erectile function.^[104][106]

Radiation therapy for prostate cancer was used occasionally in the early 20th century, with radium implanted into the urethra or rectum to reduce the tumor size and associated symptoms.^[107] In the 1950s the advent of more powerful radiation machines allowed for external beam radiotherapy to reach the prostate. By the 1960s, this was often combined with hormone therapy to improve the potency of therapy.^[107] In the 1970s, Willet Whitmore pioneered an open surgery technique where needles of Iodine-125 were placed directly into the prostate. This was improved upon by Henrik H. Holm in 1983 by using transcrectal ultrasound to guide the implantation of radioactive material.^[107]

The observation that the testicles (and the hormones they secrete) influence prostate size was made as early as the late 18th century via castration experiments in animals. However, occasional experimentation over the next century bore mixed results, likely due to the inability to separate prostate tumors from prostates enlarged due to benign prostatic hyperplasia. In 1941, Charles B. Huggins and Clarence V. Hodges published two studies using surgical castration or oral estrogen to reduce androgen levels and improve prostate cancer symptoms. Huggins was awarded the 1966 Nobel Prize in Physiology or Medicine for this discovery, the first systemic therapy for prostate cancer.^[108][109] In the 1960s, large studies showed estrogen therapy to be as effective as surgical castration at treating prostate cancer, but that those on estrogen therapy were at increased risk of suffering blood clots.^[108] Through the 1980s, Andrzej W. Schally's studies of GnRH led to the development of GnRH agonists, which were found to be as effective as estrogen without the increased risk of clotting.^[108][110] Schally was awarded the 1977 Nobel Prize in Physiology or Medicine for his work on GnRH and prostate cancer.^[108]

Systemic chemotherapy for prostate cancer has been studied since the 1950s but clinical trials failed to show benefits in most people who receive the drugs.^[111] In 1996, the US Food and Drug Administration approved the systemic chemotherapy mitoxantrone for those with castration-resistant prostate cancer based on trials showing that it improved symptoms even though it failed to enhance survival.^[112] In 2004, docetaxel was approved as the first chemotherapy to increase survival in those with castration-resistant prostate cancer.^[112] After additional trials in 2015, docetaxel use was extended to those with castration-sensitive prostate cancer.^[113]

Prostate cancer screening and awareness have been widely promoted since the early 2000s by Prostate Cancer Awareness Month in September and Movember in November.^[114] Analyses of internet searches and social media posts suggest neither event changes the level of prostate cancer interest or discussion, in contrast to the more established Breast Cancer Awareness Month.^[114][115] A light blue ribbon is used to promote prostate cancer awareness.

Prostate cancer is a major topic of ongoing research – the U.S. National Cancer Institute (NCI, the world's largest funder of cancer research) spent $209 million on prostate cancer research in 2020 – the sixth highest among cancer types.^[116] Despite high gross spending, prostate cancer research funding is relatively low for the number of deaths it causes. The NCI spends around $5,700 per prostate cancer death, considerably lower than for brain cancer ($21,000 per death), breast cancer ($13,000 per death) or cancer as a whole ($11,000 per death).^[117] A similar trend holds for private nonprofit organizations. Annual revenues of prostate cancer-focused nonprofits rank sixth among cancer types, but prostate cancer nonprofits have lower revenue than would be expected for the number of cases, deaths, and potential years of life lost.^[118]

Research into prostate cancer relies on a number of laboratory models to test aspects of the disease. Several prostate immortalized cell lines are widely used, namely the classic lines DU145, PC-3, and LNCaP, as well as more recent cell lines 22Rv1, LAPC-4, VCaP, and MDA-PCa-2a and −2b.^[119] Research requiring more complex models of the prostate uses organoids – clusters of prostate cells that can be grown from human prostate tumors or stem cells.^[120] Modeling tumor growth and metastasis requires a model organism, typically a mouse. Researchers can either surgically implant human prostate tumors into immunocompromised mice (a technique called a patient derived xenograft),^[121] or can induce prostate tumors in mice either with chemical exposure or genetic engineering.^[122] These genetically engineered mouse models typically use a Cre recombinase system to disrupt tumor suppressors or activate oncogenes specifically in prostate cells.^[123]

Works cited edit