Cancer staging
| Cancer staging | |
|---|---|
 3D medical illustration depicting the TNM stages in breast cancer | |
| Purpose | Determining the extent to which a cancer has developed |
Cancer staging is the process of determining the extent to which acancer has grown and spread. A number from I to IV is assigned, with I being an isolated cancer and IV being a cancer that has metastasized and spread from its origin. The stage generally takes into account the size of atumor, whether it has invaded adjacentorgans, how many regional (nearby)lymph nodes it has spread to (if any), and whether it has appeared in more distant locations (metastasized).
TNM staging system
Cancer staging can be divided into a clinical stage and a pathologic stage. In theTNM (Tumor, Node, Metastasis) system, clinical stage and pathologic stage are denoted by a small "c" or "p" before the stage (e.g., cT3N1M0 or pT2N0). This staging system is used for most forms of cancer, exceptbrain tumors andhematological malignancies.
- Clinical stage is based on all of the available information obtained before asurgery to remove the tumor. This stage may include information about the tumor obtained byphysical examination,blood tests,radiologic examination,biopsy, andendoscopy.
- Pathologic stage adds additional information gained by examination of the tumormicroscopically by apathologist after it has been surgically removed.
Because they use different criteria, clinical stage and pathologic stage often differ. Pathologic staging is usually considered to be more accurate because it allows direct examination of the tumor in its entirety, contrasted with clinical staging which is limited by the fact that the information is obtained by making indirect observations of a tumor which is still in the body. However, clinical staging and pathologic staging often complement each other. Not every tumor is treated surgically, so pathologic staging is not always available. Also, sometimes surgery is preceded by other treatments such aschemotherapy andradiation therapy which shrink the tumor, so the pathologic stage may underestimate the true stage.
Considerations
Correct staging is critical because treatment (particularly the need for pre-operative therapy and/or for adjuvant treatment, the extent of surgery) is generally based on this parameter. Thus, incorrect staging would lead to improper treatment.
For some common cancers the staging process is well-defined. For example, in the cases of breast cancer and prostate cancer, doctors routinely can identify that the cancer is early and that it has low risk of metastasis.[1] In such cases,medical specialtyprofessional organizations recommend against the use ofPET scans,CT scans, orbone scans because research shows that the risk of getting such procedures outweighs the possible benefits.[1] Some of the problems associated with overtesting include patients receiving invasive procedures,overutilizing medical services, getting unnecessary radiation exposure, and experiencing misdiagnosis.[1]
Pathologic
Pathologic staging, where a pathologist examines sections oftissue, can be particularly problematic for two specific reasons: visual discretion and random sampling of tissue. "Visual discretion" means being able to identify single cancerous cells intermixed with healthy cells on a slide. Oversight of onecell can mean misstaging and lead to serious, unexpected spread of cancer. "Random sampling" refers to the fact that lymph nodes are cherry-picked from patients and random samples are examined. If cancerous cells present in thelymph node happen not to be present in the slices of tissue viewed, incorrect staging and improper treatment can result.
Current research
New, highly sensitive methods of staging are in development. For example, themRNA for GCC (guanylyl cyclase c), present only in the luminal aspect ofintestinal epithelium, can be identified using molecular screening (RT-PCR) with a high degree of sensitivity and exactitude. Presence of GCC in any other tissue of the body representscolorectal metaplasia. Because of its high sensitivity, RT-PCR screening for GCC greatly reduces underestimation of disease stage. Researchers hope that staging with this level of precision will lead to more appropriate treatment and betterprognosis. Furthermore, researchers hope that this same technique can be applied to other tissue-specificproteins.
Systems
Staging systems are specific for each type of cancer (e.g.,breast cancer andlung cancer), but some cancers do not have a staging system. Although competing staging systems still exist for some types of cancer, the universally-accepted staging system is that of theUICC, which has the same definitions of individual categories as theAJCC.
Systems of staging may differ between diseases or specific manifestations of a disease.
Blood
- Lymphoma: most useAnn Arbor staging
- Hodgkin lymphoma: follows a scale from I to IV and can be indicated further by an A or B, depending on whether a patient is non-symptomatic or has symptoms such as fevers. It is known as the "Cotswold System" or "Modified Ann Arbor Staging System".[2]
Solid
For solid tumors, TNM is by far the most commonly used system, but it has been adapted for some conditions.
- Brain cancer: For most brain cancers, no staging systems are available and they are insteadgraded. Embryonal CNS tumors likemedulloblastoma are staged following a classification developed by Chang et al.[4][5]
- Breast cancer: Inbreast cancer classification, staging is usually based onTNM,[6] but staging in I–IV may be used as well.
- Cervical and ovarian cancers: the "FIGO" system has been adopted into the TNM system. For premalignant dysplastic changes, the CIN (cervical intraepithelial neoplasia) grading system is used.[7]
- Colon cancer: originally consisted of four stages: A, B, C, and D (theDukes staging system). More recently, colon cancer staging is indicated either by the original A-D stages or by TNM.[8]
- Kidney cancer: uses TNM.[9]
- Cancer of the larynx: Uses TNM.[10]
- Liver cancer: Uses TNM.[11]
- Lung cancer: uses TNM.[12]
- Melanoma: TNM used. Also of importance are the "Clark level" and "Breslow depth" which refer to the microscopic depth of tumor invasion ("Microstaging").[13]
- Prostate cancer: TNM almost universally used.[14]
- Testicular cancer: uses TNM along with a measure ofblood serum markers (TNMS).
- Non-melanoma skin cancer: uses TNM.
- Bladder cancer: uses TNM.[15]
Overall stage grouping
Overall Stage Grouping is also referred to asRoman Numeral Staging. This system uses numerals I, II, III, and IV (plus the 0) to describe the progression of cancer.
- Stage 0:carcinomain situ, abnormal cells growing in their normal place ("in situ" from Latin for "in its place").
- Stage 0 can also mean no remaining cancer afterpreoperative treatment in some cancers (e.g.colorectal cancer).
- Stage I: cancers are localized to one part of the body. Stage I cancer can be surgically removed if small enough.
- Stage II: cancers are locally advanced. Stage II cancer can be treated by chemotherapy, radiation, or surgery.
- Stage III: cancers are also locally advanced. Whether a cancer is designated as Stage II or Stage III can depend on the specific type of cancer; for example, inHodgkin's Disease, Stage II indicates affected lymph nodes on only one side of the diaphragm, whereas Stage III indicates affected lymph nodes above and below the diaphragm. The specific criteria for Stages II and III therefore differ according to diagnosis. Stage III can be treated by chemotherapy, radiation, or surgery.
- Stage IV: cancers have oftenmetastasized, or spread to other organs or throughout the body. Stage IV cancer can be treated by chemotherapy, radiation, or surgery. Despite treatment, a patient's mortality rate can be significantly higher with Stage IV cancer, e.g., the cancer can progress to becometerminal.
Within the TNM system, a cancer may also be designated as recurrent, meaning that it has appeared again after being in remission or after all visible tumor has been eliminated. Recurrence can either be local, meaning that it appears in the same location as the original, or distant, meaning that it appears in a different part of the body.
Stage migration
Stage migration is a change in the distribution of stages in a particular cancer population, induced by either a change in the staging system itself or else a change in technology which allows more sensitive detection of tumor spread and therefore more sensitivity in detecting spread of disease (e.g., the use ofMRI scans). Stage migration can lead to curious statistical phenomena (for example, theWill Rogers phenomenon).
References
- ↑1.01.11.2American Society of Clinical Oncology,"Five Things Physicians and Patients Should Question"(PDF),Choosing Wisely: an initiative of theABIM Foundation,American Society of Clinical Oncology, archived fromthe original(PDF) on July 31, 2012, retrievedAugust 14, 2012, citing
- Carlson, R. W.; Allred, D. C.; Anderson, B. O.; Burstein, H. J.; Carter, W. B.; Edge, S. B.; Erban, J. K.; Farrar, W. B.; Goldstein, L. J.; Gradishar, W. J.; Hayes, D. F.; Hudis, C. A.; Jahanzeb, M.; Kiel, K.; Ljung, B. M.; Marcom, P. K.; Mayer, I. A.; McCormick, B.; Nabell, L. M.; Pierce, L. J.; Reed, E. C.; Smith, M. L.; Somlo, G.; Theriault, R. L.; Topham, N. S.; Ward, J. H.; Winer, E. P.; Wolff, A. C.; NCCN Breast Cancer Clinical Practice Guidelines Panel (2009)."Breast cancer. Clinical practice guidelines in oncology".Journal of the National Comprehensive Cancer Network.7 (2): 122–192.doi:10.6004/jnccn.2009.0012.PMID 19200416.
- Thompson, I.; Thrasher, J. B.; Aus, G.; Burnett, A. L.; Canby-Hagino, E. D.; Cookson, M. S.; d'Amico, A. V.; Dmochowski, R. R.; Eton, D. T.; Forman, J. D.; Goldenberg, S. L.; Hernandez, J.; Higano, C. S.; Kraus, S. R.; Moul, J. W.; Tangen, C. M.; AUA Prostate Cancer Clinical Guideline Update Panel (2007). "Guideline for the Management of Clinically Localized Prostate Cancer: 2007 Update".The Journal of Urology.177 (6): 2106–2131.doi:10.1016/j.juro.2007.03.003.PMID 17509297.
- ↑"Hodgkin's Disease - Staging". oncologychannel. Archived fromthe original on 2008-10-25. Retrieved2010-10-14.
- ↑Casal-Mouriño, Ana; Ruano-Ravina, Alberto; Lorenzo-González, María; Rodríguez-Martínez, Ángeles; Giraldo-Osorio, Alexandra; Varela-Lema, Leonor; Pereiro-Brea, Tara; Barros-Dios, Juan Miguel; Valdés-Cuadrado, Luis; Pérez-Ríos, Mónica (January 2021)."Epidemiology of stage III lung cancer: frequency, diagnostic characteristics, and survival".Translational Lung Cancer Research.10 (1): 506–518.doi:10.21037/tlcr.2020.03.40.ISSN 2218-6751.Archived from the original on 2024-08-24. Retrieved2024-08-22.
- ↑Central Nervous System Tumours. International Agency for Research on Cancer. 2021.ISBN 9789283245087.
- ↑Chang, Chu H.; Housepian, Edgar M.; Herbert, Charles (1969)."An Operative Staging System and a Megavoltage Radiotherapeutic Technic for Cerebellar Medulloblastomas".Radiology.93 (6): 1351–1359.doi:10.1148/93.6.1351.ISSN 0033-8419.PMID 4983156.Archived from the original on 2024-08-24. Retrieved2024-08-08.
- ↑"Breast Cancer Treatment - National Cancer Institute". Cancer.gov. 2010-08-13.Archived from the original on 2015-04-04. Retrieved2010-10-14.
- ↑Eric Lucas (2006-01-31)."FIGO staging of cervical carcinomas". Screening.iarc.fr. Archived fromthe original on 2008-10-24. Retrieved2010-10-14.
- ↑"Colon Cancer - Staging". oncologychannel. Archived fromthe original on 2008-10-24. Retrieved2010-10-14.
- ↑"Stages of kidney cancer". Cancerhelp.org.uk. 2010-06-30. Archived fromthe original on 2009-01-22. Retrieved2010-10-14.
- ↑"The stages of cancer of the larynx". Cancerhelp.org.uk. 2010-07-28. Archived fromthe original on 2008-12-16. Retrieved2010-10-14.
- ↑"How is liver cancer staged?". Archived fromthe original on 2016-12-03. Retrieved2013-06-02.
- ↑Imaging in Lung Cancer Staging ateMedicine
- ↑"malignant melanoma: staging". Chorus.rad.mcw.edu. Archived fromthe original on 2010-07-18. Retrieved2010-10-14.
- ↑"NCCN Guidelines for Patients". National Comprehensive Cancer Network. Archived fromthe original on 2015-10-25. Retrieved2015-11-01.
- ↑"Bladder Cancer Stages".Cancer.org.American Cancer Society.Archived from the original on 30 December 2017. Retrieved29 December 2017.