Colon Cancer Staging 

No Results

No Results

processing….

The American Joint Committee on Cancer (AJCC) tumor/node/metastasis (TNM) classification and staging system for colon cancer are provided below. ^{[1, 2]}

See Benign or Malignant: Can You Identify These Colonic Lesions?, a Critical Images slideshow, to help identify the features of benign lesions as well as those with malignant potential.

Table 1. TNM Classification for Colon Cancer (Open Table in a new window)

Primary tumor (T)

TX

Primary tumor cannot be assessed

T0

No evidence of primary tumor

Tis

Carcinoma in situ: intraepithelial or or intramucosal carcinoma (involvement of lamina propria with no extension through the muscularis mucosa)

T1

Tumor invades submucosa (through the muscularis mucosa but not into the muscularis propria)

T2

Tumor invades muscularis propria

T3

Tumor invades through the muscularis propria into the pericolorectal tissues

T4

Tumor invades the visceral peritoneum or invades or adheres to adjacent organ or structure

T4a

Tumor invades through the visceral peritoneum (including gross perforation of the bowel through tumor and continuous invasion of tumor through areas of inflammation to the surface of the visceral peritoneum)

T4b

Tumor directly invades or is adherent to other organs or structures

Regional lymph nodes (N)

NX

Regional lymph nodes cannot be assessed

N0

No regional lymph node metastasis

N1

Metastasis in 1-3 regional lymph nodes (tumor in lymph nodes measuring ≥0.2 mm) or any number of tumor deposits are present and all identifiable nodes are negative

N1a

Metastasis in 1 regional lymph node

N1b

Metastasis in 2-3 regional lymph nodes

N1c

Tumor deposit(s) in the subserosa, mesentery, or nonperitonealized, pericolic, or perirectal/mesorectal tissues without regional nodal metastasis

N2

Metastasis in 4 or more lymph nodes

N2a

Metastasis in 4-6 regional lymph nodes

N2b

Metastasis in 7 or more regional lymph nodes

Distant metastasis (M)

M0

No distant metastasis by imaging or other studies, no evidence of tumor in distant sites or organs. (This category is not assigned by pathologists.)

M1

Metastasis to one or more distant sites or organs or peritoneal metastasis

M1a

Metastasis confined to 1 organ or site (eg, liver, lung, ovary, nonregional node) without peritoneal metastasis

M1b

Metastasis to two or more sites or organs without peritoneal metastasis

M1c

Metastasis to the peritoneal surface alone or with other site or organ metastases

Table 2. Anatomic stage/prognostic groups (Open Table in a new window)

Stage

T

N

M

Dukes

MAC

0

Tis

N0

M0

—

—

I

T1

N0

M0

A

A

T2

N0

M0

A

B1

IIA

T3

N0

M0

B

B2

IIB

T4a

N0

M0

B

B2

IIC

T4b

N0

M0

B

B3

IIIA

T1-T2

N1/N1c

M0

C

C1

T1

N2a

M0

C

C1

IIIB

T3-T4a

N1/N1c

M0

C

C2

T2-T3

N2a

M0

C

C1/C2

T1-T2

N2b

M0

C

C1

IIIC

T4a

N2a

M0

C

C2

T3-T4a

N2b

M0

C

C2

T4b

N1-N2

M0

C

C3

IVA

Any T

Any N

M1a

—

—

IVB

IVC

Any T

Any T

Any N

Any T

M1b

M1c

—

—

Staging information

Compared with the 7th edition of the AJCC staging manual, features of revised staging in the 8th edition give more importance to the poor prognostic features of depth of invasion in spite of fewer positive nodes.

T4 is divided between penetration to surface of visceral peritoneum and direct gross adherence to adjacent structures

T1-2N2 is downstaged from stage IIIC to IIIA or IIIB, depending on the number of nodes involved

Shift T4bN1 from IIIB to IIIC

Subdivide T4/N1/N2

Resolution of staging for issue of mesenteric deposits where nodal tissue is not identified

Revised substaging of stage II based on depth of invasion, with addition of stage IIC

Revised substaging of stage III based on node number (N1a—1 node; N1b—2-3 nodes; N2a—4-6 nodes; N2b—7 or more nodes)

Division of metastases to 1 or more sites in recognition of possibility of cure with aggressive treatment of single site of metastatic disease

Stage M1c has been introduced to represent the poor prognosis of peritoneal carcinomatosis.

Nodal micrometastases (tumor clusters ≥0.2 mm in diameter) are now scored as positive due to results of meta-analysis demonstrating poor prognosis in these patients. ^[3]

Other tumor deposits in peritoneum, subserosa, and mesentery are given equal weight as nodal metastases.

The following factors are important in determining treatment decisions but are not yet incorporated into the formal staging criteria:

A preoperative serum carcinoembryonic antigen(CEA) levels

Tumor regression score reflective of pathologic response to preoperative chemotherapy, chemoradiotherapy, radiotherapy, or chemobiologic therapy as well as status of circumferential margin for rectal cancer.

Lymphovascular and perineural invasion

Microsatellite instability (MSI), which represents deficiency of mismatch repair enzymes and is both a progostic factor and predictive of lack of response to fluoropyrimidine therapy in the adjuvant setting.

Mutation status of KRAS, NRAS, and BRAF, because mutations in those genes are associated with lack of response to agents targeting epidermal growth factor receptors.  

[Guideline] NCCN Clinical Practice Guidelines in Oncology: Colon Cancer. National Comprehensive Cancer Network. Available at http://www.nccn.org/professionals/physician_gls/pdf/colon.pdf. Version 2.2017 — March 13, 2017; Accessed: January 9, 2018.

American Joint Committee on Cancer. Colon and Rectum. Amin MB, Edge S, Greene F, Byrd DR, Brookland RK, et al, eds. AJCC Cancer Staging Manual. 8th ed. New York, NY: Springer; 2016.

Sloothaak DA, Sahami S, van der Zaag-Loonen HJ, van der Zaag ES, Tanis PJ, Bemelman WA, et al. The prognostic value of micrometastases and isolated tumour cells in histologically negative lymph nodes of patients with colorectal cancer: a systematic review and meta-analysis. Eur J Surg Oncol. 2014 Mar. 40 (3):263-9. [Medline].

Primary tumor (T)

TX

Primary tumor cannot be assessed

T0

No evidence of primary tumor

Tis

Carcinoma in situ: intraepithelial or or intramucosal carcinoma (involvement of lamina propria with no extension through the muscularis mucosa)

T1

Tumor invades submucosa (through the muscularis mucosa but not into the muscularis propria)

T2

Tumor invades muscularis propria

T3

Tumor invades through the muscularis propria into the pericolorectal tissues

T4

Tumor invades the visceral peritoneum or invades or adheres to adjacent organ or structure

T4a

Tumor invades through the visceral peritoneum (including gross perforation of the bowel through tumor and continuous invasion of tumor through areas of inflammation to the surface of the visceral peritoneum)

T4b

Tumor directly invades or is adherent to other organs or structures

Regional lymph nodes (N)

NX

Regional lymph nodes cannot be assessed

N0

No regional lymph node metastasis

N1

Metastasis in 1-3 regional lymph nodes (tumor in lymph nodes measuring ≥0.2 mm) or any number of tumor deposits are present and all identifiable nodes are negative

N1a

Metastasis in 1 regional lymph node

N1b

Metastasis in 2-3 regional lymph nodes

N1c

Tumor deposit(s) in the subserosa, mesentery, or nonperitonealized, pericolic, or perirectal/mesorectal tissues without regional nodal metastasis

N2

Metastasis in 4 or more lymph nodes

N2a

Metastasis in 4-6 regional lymph nodes

N2b

Metastasis in 7 or more regional lymph nodes

Distant metastasis (M)

M0

No distant metastasis by imaging or other studies, no evidence of tumor in distant sites or organs. (This category is not assigned by pathologists.)

M1

Metastasis to one or more distant sites or organs or peritoneal metastasis

M1a

Metastasis confined to 1 organ or site (eg, liver, lung, ovary, nonregional node) without peritoneal metastasis

M1b

Metastasis to two or more sites or organs without peritoneal metastasis

M1c

Metastasis to the peritoneal surface alone or with other site or organ metastases

Stage

T

N

M

Dukes

MAC

0

Tis

N0

M0

—

—

I

T1

N0

M0

A

A

T2

N0

M0

A

B1

IIA

T3

N0

M0

B

B2

IIB

T4a

N0

M0

B

B2

IIC

T4b

N0

M0

B

B3

IIIA

T1-T2

N1/N1c

M0

C

C1

T1

N2a

M0

C

C1

IIIB

T3-T4a

N1/N1c

M0

C

C2

T2-T3

N2a

M0

C

C1/C2

T1-T2

N2b

M0

C

C1

IIIC

T4a

N2a

M0

C

C2

T3-T4a

N2b

M0

C

C2

T4b

N1-N2

M0

C

C3

IVA

Any T

Any N

M1a

—

—

IVB

IVC

Any T

Any T

Any N

Any T

M1b

M1c

—

—

Lewis J Rose, MD Clinical Associate Professor of Medical Oncology, Division of Regional Cancer Care, Kimmel Cancer Center, Thomas Jefferson University Hospital; Consulting Staff, LRCRZ Associates

Lewis J Rose, MD is a member of the following medical societies: American College of Physicians, American Medical Association, American Society of Hematology, Pennsylvania Medical Society, Phi Beta Kappa, Philadelphia County Medical Society

Disclosure: Nothing to disclose.

Jasmeet Anand, PharmD, RPh Adjunct Instructor, University of Nebraska Medical Center College of Pharmacy; Editor-in-Chief, Medscape Drug Reference

Disclosure: Nothing to disclose.

Christopher D Braden, DO Hematologist/Oncologist, Chancellor Center for Oncology at Deaconess Hospital; Medical Director, Deaconess Hospital Outpatient Infusion Centers; Chairman, Deaconess Hospital Cancer Committee

Christopher D Braden, DO is a member of the following medical societies: American Society of Clinical Oncology, American Society of Hematology

Disclosure: Nothing to disclose.

N Joseph Espat, MD, MS, FACS Harold J Wanebo Professor of Surgery, Assistant Dean of Clinical Affairs, Boston University School of Medicine; Chairman, Department of Surgery, Director, Adele R Decof Cancer Center, Roger Williams Medical Center

N Joseph Espat, MD, MS, FACS is a member of the following medical societies: Alpha Omega Alpha, American Association for Cancer Research, American College of Surgeons, American Medical Association, American Society for Parenteral and Enteral Nutrition, American Society of Clinical Oncology, Americas Hepato-Pancreato-Biliary Association, Association for Academic Surgery, Central Surgical Association, Chicago Medical Society, International Hepato-Pancreato-Biliary Association, Pancreas Club, Sigma Xi, Society for Leukocyte Biology, Society for Surgery of the Alimentary Tract, Society of American Gastrointestinal and Endoscopic Surgeons, Society of Surgical Oncology, Society of University Surgeons, Southeastern Surgical Congress, Southern Medical Association, Surgical Infection Society

Disclosure: Nothing to disclose.

Colon Cancer Staging 

Research & References of Colon Cancer Staging |A&C Accounting And Tax Services
Source

Share on Facebook

Tweet

Follow us