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Serum tumor markers
tool for the management of cancer

DR.PANKAJ GUPTA
OBJECTIVES

• What are they?
• Why are they used?

• How are they used?
A BREIF HISTORY OF TUMOR MARKERS
• In 1875, H. Bence Jones described and named Multiple Myeloma
and Bence Jones Proteinuria
• In 1960, immunoassay techniques were developed

• In 1975, monoclonal antibodies were developed by hybridoma
technique
TUMOUR MARKERS: A DEFINITION
“Tumour markers are molecules that can be detected in blood,
body fluids or tissue of the host and which are produced either as
a response to cancer or by cancer cells themselves.”
WHAT MAKES AN IDEAL TUMOR MARKER ?
• 100% sensitive and specific

• Having a short half life
• Easily measurable and easily reproducible
• Proportionate to the size of the tumour
• Cost-effective
CLASSIFICATION
Tumour
markers

Tumour
associated
proteins

Oncofetal
antigens

Epithelial
antigens

Oncoproteins/
Oncogenes

Enzymes

Hormones

Tumour
suppressor
genes

Adhesion
molecules
CLINICAL IMPLICATION

Screening

Diagnosis

Staging

Prognosis

Monitoring
treatment

Recurrence
RECONMENDATIONS FOR ORDERING
TUMORS MARKES
• Do serial testing
• Same lab

• While monitoring recurrence, make sure the tumour marker level was
elevated before surgery
• Considering half life while interpreting the result
• Know the metabolism of the tumour marker
• Panel testing is better than testing a single marker
α- FETO PROTEIN (AFP)
• Glycoprotein
• Secreted from fetal yolk sac, liver and gastrointestinal tract

• Normal levels are <15 ng/ml (HL= 3-5 days)
• Resembles, structurally as well as genetically to albumin
INTERPRETATION
1. Hepatocellular carcinoma
• Screening tool in high prevalence areas

• Levels > 500 ng/ml in adults
• Markedly increased levels (>1000 ng/ml) s/o tumors size > 3cm

• High initial concentrations correlate with poor prognosis
• Failure to return normal after surgery indicates incomplete resection
or presence of mets
• Post operative decrease in concentration followed by increase
suggest recurrence

• Short doubling time usually is predictor of occult metastasis
2. Tumor marker for germ cell tumors of ovary and testis
• Embryonal carcinoma
• Malignant teratoma
3. Can also be increased in
• Pancreatic, gastric, bronchogenic and colon cancer
• Benign disease like hepatitis, post necrotic cirrhosis, primary biliary
cirrhosis.

4. Neonatal hepatitis and neonatal biliary atresia.
5. Screening for fetal defects and placental diseases
CARCINOMA EMBRYONIC ANTIGEN (CEA)
• High molecular weight glycoprotein

• Normal value is <2.5ng/ml
• Half life 3-13 days

• Has a diagnostic and prognostic importance in colorectal cancer
• Lacks high sensitivity and specificty
INTERPRETATION
In Colon cancer
• After complete removal of colon cancer, the levels should fall to
normal in 6-12 weeks.

• CEA has sensitivity of 97% in detecting recurrence in patients with
preoperative elevated levels
• Increase concentration indicates poor prognosis within a given
stage
• High level correlate with metastasis (80% patient of colon cancer
with level > 20 ng/ml have recurrence in 14 months)
• Concentrations < 5ng/ml before therapy correlate with localized
disease and good prognosis
• Uninterrupted increase denote failure to response
• Immediate sustained decrease followed by increase indicate, lack of
response
• Undifferentiated or poorly differentiated tumors do not produce
CEA
• Levels <2.5 ng/ml do not rule out primary, metastatic or recurrent
cancer
• Surge in CEA for weeks followed by decrease indicate response
Increased in
• Cancers of Stomach, Pancreas, Lung, Breast, Head and neck and
ovary

• Effusion fluids due to these cancers
• Active non malignant inflammatory diseases like UC, peptic ulcers,
regional enteritis, chronic pancreatitis

• Liver diseases, Renal failure, Heavy smokers
CA-125
• A mucin-like glycoprotein with a molecular weight of 200kDa
recognized by monoclonal antibody OC 125
• Normal value <35 U/ml
• Has a half -life of 3-5days
• Elevated in more than 80% of non-mucinous ovarian cancer
INTERPREATION
• Normal concentrations does not exclude tumor
• Not useful in distinguish benign and malignant pelvic mass
• Not recommended for screening women for serous carcinomas of ovary
• May be useful for screening in hereditary cancer syndrome

• Correlates with poorer prognosis if elevated 3-6 weeks after surgery
• Concentration of > 35 U/ml detects residual tumor in 95 % patients but
normal levels do not exclude
• Rising levels during chemotherapy is associated with tumor
progression and fall to normal is associated with response
• Rising concentration may precede clinical recurrence by many months
but normal levels does not indicate absence of persistent or recurrent
tumor

• Values > 65 U/ml correlate with peritoneal involvement
• Prognosis may be better if
1. 50% decline within 5 days of surgery
2. Ratio of postoperative and preoperative concentrations (4 weeks)

3. Ratio >0.1 to <0.5 may benefit from chemotherapy
4. Ratio > 0.8 should consider alternative therapy
Increased in
• Non mucinous epithelial ovarian carcinoma (85%) and Tumors of
Fallopian tube (100%)
• Cervical adenocarcinoma, Endometrial adenocarcinoma,
Trophoblastic tumors, liver, lung and pancreas
• Non hodgkin lymphomas representing pleuropericardial or peritoneal
involvement
• Cirrhosis, Renal failure, Menstruation, Endometriosis, disorders of
GI tract
HUMAN CHORIONIC GONADOTROPHIN
(hCG)
• A glycoprotein hormone synthesized by placenta

• Has alpha and beta subunits
• Normal value of beta hCG is<5mIU/ml
• Normal half-life of 12-20hrs
• Used as a routine pregnancy test
• Diagnosis and monitor course and evaluate prognosis of gestational
trophoblastic tumors (with AFP)
• Differentiation of ectopic pregnancy from other causes of acute
abdomen
• Prenatal screening of Down syndrome
• Increased levels after 12 weeks of pregnancy >500,000 IU/24 hours
usually are associated with moles and level >1,000,000 IU are alsmot
always associated with moles.
• In choriocarcinoma failure to fall to an undetectable level or a rise
after initial fall, signals residual tumor
• Also increased in non seminomatous germ cell tumors of testis, some
non trophoblastic cancer like ovary, GI tract, lung and breast.
PROSTATE SPECIFIC ANTIGEN (PSA)
• Also known as human kallikrein 3

• Serine protease produced by prostatic acinar cells
• Also by periurethral glands and breast in women, pancreas and
salivary glands in both sex
•

Reference rang <4ng/ml with half life of 4 days
INTERPRETATION
• Recommended for screening along with DRE
• Used in staging of prostate cancer
- < 4ng/ml, organ confined disease
- < 10ng/ml, bone metastasis is rare
- > 10ng/ml, >50% have extracapsular disease
- > 50ng/ml, most have positive lymphnodes
- >100ng/ml, predicts bone mets with 90% accuracy, S/S=66%/96%
with a PPV = 79%.
• Failure of radiation to decrease PSA to < 1ng/ml means likelihood of
recurrence
• After radical prostatectomy doubling time reflects aggressiveness of
original cancer
• Free PSA and complex PSA help in differentiating cancer from BPH
and prostatitis
PSA velocity and density
• More rapid rate of increase of velocity (>0.75 ng/ml/year or
>20%/year) correlates with cancer. Requires min. 3 tests/18 months.
• Specially useful when PSA levels are between 4-10ng/ml

• Low density is unlikely to be cancer (<0.15)
• DRE increases PSA significantly if initial value is >20ng/ml
• PSA has no circadian rhythm but variation can occur between
specimens collected on same day
• Ejaculation causes transient increase < 1.0 ng/ml for 48 hrs
• Slight increase may be associated with cancer of salivary gland, sweat
glands, breast, colon, lung and ovary and in conditions like ARF and
MI

• Indwelling catheters, vigorous bicycle exercise, Treadmill stress test
CA 19-9
• Blood group carbohydrate
• Sialylated derivative of Lewis antigen, and is denoted a Lexa

• Synthesized by normal human pancreatic and biliary ductal cells
• Also by gastric, colonic, endometrial and salivary epithelia
• Normal value <37 U/ml
INTERPRETATION
• Used in detection, diagnosis and prognosis of pancreatic cancer
• To determine preoperative resectability

• Only 5 % of patient with levels >1000 U/ml are surgically resectable
• Post surgical increase concentration correlates with recurrence
• May indicate development of Cholangiocarcinoma in PSC
CA 15-3
• Glycoprotein expressed by various adenocarcinoma especially
breast
• Half life of around 7 days
• Only to detect breast carcinoma recurrence and to monitor
response to treatment (FDA)
INTERPRETATION
• Increases directly related to stage of disease

• Increases in 75% with progressive disease
• Decreases in 38% responding to therapy
• >30 U/L indicates shorter survival
• Also increased in benign breast disease and liver disease
CA 72-4
• A high molecular weight (>106 Da) mucin-like complex
• Marker for carcinomas of the GI tract and of the ovary
• Also used in multivariate analysis of colorectal cancer with βhcg and
CEA for prognosis
NEXT SESSION
•
•
•
•
•
•
•

Beta 2 microglobulin
Calcitonin
CYFRA 21-1
Her 2 neu
Chromagranin A
PTHRP
p53
THANK YOU

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SERUM TUMOR MARKERS

  • 1. Serum tumor markers tool for the management of cancer DR.PANKAJ GUPTA
  • 2. OBJECTIVES • What are they? • Why are they used? • How are they used?
  • 3. A BREIF HISTORY OF TUMOR MARKERS • In 1875, H. Bence Jones described and named Multiple Myeloma and Bence Jones Proteinuria • In 1960, immunoassay techniques were developed • In 1975, monoclonal antibodies were developed by hybridoma technique
  • 4. TUMOUR MARKERS: A DEFINITION “Tumour markers are molecules that can be detected in blood, body fluids or tissue of the host and which are produced either as a response to cancer or by cancer cells themselves.”
  • 5. WHAT MAKES AN IDEAL TUMOR MARKER ? • 100% sensitive and specific • Having a short half life • Easily measurable and easily reproducible • Proportionate to the size of the tumour • Cost-effective
  • 8. RECONMENDATIONS FOR ORDERING TUMORS MARKES • Do serial testing • Same lab • While monitoring recurrence, make sure the tumour marker level was elevated before surgery
  • 9. • Considering half life while interpreting the result • Know the metabolism of the tumour marker • Panel testing is better than testing a single marker
  • 10. α- FETO PROTEIN (AFP) • Glycoprotein • Secreted from fetal yolk sac, liver and gastrointestinal tract • Normal levels are <15 ng/ml (HL= 3-5 days) • Resembles, structurally as well as genetically to albumin
  • 11. INTERPRETATION 1. Hepatocellular carcinoma • Screening tool in high prevalence areas • Levels > 500 ng/ml in adults • Markedly increased levels (>1000 ng/ml) s/o tumors size > 3cm • High initial concentrations correlate with poor prognosis
  • 12. • Failure to return normal after surgery indicates incomplete resection or presence of mets • Post operative decrease in concentration followed by increase suggest recurrence • Short doubling time usually is predictor of occult metastasis
  • 13. 2. Tumor marker for germ cell tumors of ovary and testis • Embryonal carcinoma • Malignant teratoma 3. Can also be increased in • Pancreatic, gastric, bronchogenic and colon cancer • Benign disease like hepatitis, post necrotic cirrhosis, primary biliary cirrhosis. 4. Neonatal hepatitis and neonatal biliary atresia. 5. Screening for fetal defects and placental diseases
  • 14. CARCINOMA EMBRYONIC ANTIGEN (CEA) • High molecular weight glycoprotein • Normal value is <2.5ng/ml • Half life 3-13 days • Has a diagnostic and prognostic importance in colorectal cancer • Lacks high sensitivity and specificty
  • 15. INTERPRETATION In Colon cancer • After complete removal of colon cancer, the levels should fall to normal in 6-12 weeks. • CEA has sensitivity of 97% in detecting recurrence in patients with preoperative elevated levels • Increase concentration indicates poor prognosis within a given stage
  • 16. • High level correlate with metastasis (80% patient of colon cancer with level > 20 ng/ml have recurrence in 14 months) • Concentrations < 5ng/ml before therapy correlate with localized disease and good prognosis • Uninterrupted increase denote failure to response • Immediate sustained decrease followed by increase indicate, lack of response
  • 17. • Undifferentiated or poorly differentiated tumors do not produce CEA • Levels <2.5 ng/ml do not rule out primary, metastatic or recurrent cancer • Surge in CEA for weeks followed by decrease indicate response
  • 18. Increased in • Cancers of Stomach, Pancreas, Lung, Breast, Head and neck and ovary • Effusion fluids due to these cancers • Active non malignant inflammatory diseases like UC, peptic ulcers, regional enteritis, chronic pancreatitis • Liver diseases, Renal failure, Heavy smokers
  • 19. CA-125 • A mucin-like glycoprotein with a molecular weight of 200kDa recognized by monoclonal antibody OC 125 • Normal value <35 U/ml • Has a half -life of 3-5days • Elevated in more than 80% of non-mucinous ovarian cancer
  • 20. INTERPREATION • Normal concentrations does not exclude tumor • Not useful in distinguish benign and malignant pelvic mass • Not recommended for screening women for serous carcinomas of ovary • May be useful for screening in hereditary cancer syndrome • Correlates with poorer prognosis if elevated 3-6 weeks after surgery
  • 21. • Concentration of > 35 U/ml detects residual tumor in 95 % patients but normal levels do not exclude • Rising levels during chemotherapy is associated with tumor progression and fall to normal is associated with response • Rising concentration may precede clinical recurrence by many months but normal levels does not indicate absence of persistent or recurrent tumor • Values > 65 U/ml correlate with peritoneal involvement
  • 22. • Prognosis may be better if 1. 50% decline within 5 days of surgery 2. Ratio of postoperative and preoperative concentrations (4 weeks) 3. Ratio >0.1 to <0.5 may benefit from chemotherapy 4. Ratio > 0.8 should consider alternative therapy
  • 23. Increased in • Non mucinous epithelial ovarian carcinoma (85%) and Tumors of Fallopian tube (100%) • Cervical adenocarcinoma, Endometrial adenocarcinoma, Trophoblastic tumors, liver, lung and pancreas • Non hodgkin lymphomas representing pleuropericardial or peritoneal involvement • Cirrhosis, Renal failure, Menstruation, Endometriosis, disorders of GI tract
  • 24. HUMAN CHORIONIC GONADOTROPHIN (hCG) • A glycoprotein hormone synthesized by placenta • Has alpha and beta subunits • Normal value of beta hCG is<5mIU/ml • Normal half-life of 12-20hrs
  • 25. • Used as a routine pregnancy test • Diagnosis and monitor course and evaluate prognosis of gestational trophoblastic tumors (with AFP) • Differentiation of ectopic pregnancy from other causes of acute abdomen • Prenatal screening of Down syndrome
  • 26. • Increased levels after 12 weeks of pregnancy >500,000 IU/24 hours usually are associated with moles and level >1,000,000 IU are alsmot always associated with moles. • In choriocarcinoma failure to fall to an undetectable level or a rise after initial fall, signals residual tumor • Also increased in non seminomatous germ cell tumors of testis, some non trophoblastic cancer like ovary, GI tract, lung and breast.
  • 27. PROSTATE SPECIFIC ANTIGEN (PSA) • Also known as human kallikrein 3 • Serine protease produced by prostatic acinar cells • Also by periurethral glands and breast in women, pancreas and salivary glands in both sex • Reference rang <4ng/ml with half life of 4 days
  • 28. INTERPRETATION • Recommended for screening along with DRE • Used in staging of prostate cancer - < 4ng/ml, organ confined disease - < 10ng/ml, bone metastasis is rare - > 10ng/ml, >50% have extracapsular disease - > 50ng/ml, most have positive lymphnodes - >100ng/ml, predicts bone mets with 90% accuracy, S/S=66%/96% with a PPV = 79%.
  • 29. • Failure of radiation to decrease PSA to < 1ng/ml means likelihood of recurrence • After radical prostatectomy doubling time reflects aggressiveness of original cancer • Free PSA and complex PSA help in differentiating cancer from BPH and prostatitis
  • 30.
  • 31. PSA velocity and density • More rapid rate of increase of velocity (>0.75 ng/ml/year or >20%/year) correlates with cancer. Requires min. 3 tests/18 months. • Specially useful when PSA levels are between 4-10ng/ml • Low density is unlikely to be cancer (<0.15)
  • 32. • DRE increases PSA significantly if initial value is >20ng/ml • PSA has no circadian rhythm but variation can occur between specimens collected on same day • Ejaculation causes transient increase < 1.0 ng/ml for 48 hrs • Slight increase may be associated with cancer of salivary gland, sweat glands, breast, colon, lung and ovary and in conditions like ARF and MI • Indwelling catheters, vigorous bicycle exercise, Treadmill stress test
  • 33. CA 19-9 • Blood group carbohydrate • Sialylated derivative of Lewis antigen, and is denoted a Lexa • Synthesized by normal human pancreatic and biliary ductal cells • Also by gastric, colonic, endometrial and salivary epithelia • Normal value <37 U/ml
  • 34. INTERPRETATION • Used in detection, diagnosis and prognosis of pancreatic cancer • To determine preoperative resectability • Only 5 % of patient with levels >1000 U/ml are surgically resectable • Post surgical increase concentration correlates with recurrence • May indicate development of Cholangiocarcinoma in PSC
  • 35. CA 15-3 • Glycoprotein expressed by various adenocarcinoma especially breast • Half life of around 7 days • Only to detect breast carcinoma recurrence and to monitor response to treatment (FDA)
  • 36. INTERPRETATION • Increases directly related to stage of disease • Increases in 75% with progressive disease • Decreases in 38% responding to therapy • >30 U/L indicates shorter survival • Also increased in benign breast disease and liver disease
  • 37. CA 72-4 • A high molecular weight (>106 Da) mucin-like complex • Marker for carcinomas of the GI tract and of the ovary • Also used in multivariate analysis of colorectal cancer with βhcg and CEA for prognosis
  • 38. NEXT SESSION • • • • • • • Beta 2 microglobulin Calcitonin CYFRA 21-1 Her 2 neu Chromagranin A PTHRP p53