| Literature DB >> 23431473 |
Abstract
The role of surgeons in the treatment of Merkel cell carcinoma (MCC) of the skin is reviewed, with respect to diagnosis and treatment. Most of the data in the literature are case reports. Surgery is the mainstay of treatment. A wide local excision, with sentinel node (SLN) biopsy, is the recommended treatment of choice. If SLN is involved, nodal dissection should be performed; unless patient is unfit, then regional radiotherapy can be given. Surgeons should always refer patients for assessment of the need for adjuvant treatments. Adjuvant radiotherapy is well tolerated and effective to minimize recurrence. Adjuvant chemotherapy may be considered for selected node-positive patients, as per National Comprehensive Cancer Network guideline. Data are insufficient to assess whether adjuvant chemotherapy improves survival. Recurrent disease should be treated by complete surgical resection if possible, followed by radiotherapy and possibly chemotherapy. Generally results of multimodality treatment for recurrent disease are better than lesser treatments. Future research should focus on newer chemotherapy and molecular targeted agents in the adjuvant setting and for gross disease.Entities:
Year: 2013 PMID: 23431473 PMCID: PMC3570924 DOI: 10.1155/2013/850797
Source DB: PubMed Journal: ISRN Surg ISSN: 2090-5785
Pathology diagnosis of MCC.
| (1) Perform fine needle aspiration cytology or biopsy of different lesions in the same patient. | |
| (2) Section skin specimen thoroughly to avoid missing the aggressive MCC component since it can coexist with other more common skin cancers. | |
| (3) Immunostaining for cytokeratin-20 can detect micrometastasis in sentinel nodes. |
Summary of the 2010 American Joint Committee on Cancer Merkel Cell Carcinoma staging system.
| Primary tumor (T) | |
|---|---|
| Tx | Primary tumor cannot be assessed |
| T0 | No evidence of primary tumor |
| Tis | In situ primary tumor |
| T1 | Primary tumors less than or equal to 2 cm maximum tumor dimension |
| T2 | Primary tumors greater than 2 cm but not more than 5 cm maximum tumor dimension |
| T3 | Primary tumors over 5 cm maximum tumor dimension |
| T4 | Primary tumor invades bone, muscle, fascia, or cartilage |
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| Regional lymph nodes (N) | |
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| Nx | Regional lymph nodes cannot be assessed |
| N0 | No regional lymph node metastasis |
| cN0 | Nodes negative by clinical exam (no pathologic node exam performed) |
| pN0 | Nodes negative by pathologic exam |
| N1 | Metastasis in regional lymph node(s) |
| N1a | Micrometastasis |
| N1b | Macrometastasis |
| N2 | In-transit metastasis |
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| Distant metastasis (M) | |
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| M0 | No distant metastasis |
| M1 | Metastasis beyond regional lymph nodes |
| M1a | Metastasis to skin, subcutaneous tissues, or distant lymph nodes |
| M1b | Metastasis to lung |
| M1c | Metastasis to all other visceral sites |
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| Anatomic stage/prognostic groups | |
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| IA | Primary tumor ≤2 cm; regional LN negative by pathologic examinationa |
| IB | Primary tumor ≤2 cm; regional LN negative by clinical examination onlyb |
| IIA | Primary tumor >2 cm; regional LN negative by pathologic examinationa |
| IIB | Primary tumor >2 cm; regional LN negative by clinical examination onlyb |
| IIIA | Primary tumor any size; positive micrometastasis in regional LNc |
| IIIB | Primary tumor any size; clinically detectable regional LN metastasis and/or in-transit metastasisd |
| IV | Primary tumor any size; any distant metastasis |
aNegative sentinel lymph node biopsy (SLNB) or elective lymph node dissection (ELND).
bNo pathologic LN evaluation (SLNB or ELND).
cPositive micrometastasis by SLNB or ELND.
dConfirmed pathologically by biopsy or therapeutic lymph node dissection.
LN: lymph nodes.
5-year survival outcome of different stages of MCC [7].
| Percentage of all patients | 5-year overall survival | |
|---|---|---|
| Stage I and II (localized disease) | 60%–70% | 60%–80% |
| Stage III (nodal disease) | 30% | 50% |
| Stage IV (distant metastasis) | 5%–10% | 20% |
| All stages combined | 100% | 40% |
Staging workup should include the following.
| (1) Complete examination of the skin (including scalp) and regional lymph nodes | |
| (2) Computerized tomography (CT) of chest to rule out lung metastases or small-cell carcinoma arising in the lung and metastasizing to the skin | |
| (3) Positron emission tomography (PET) with 18-fluorodeoxyglucose (18FDG), either alone or combined with computed tomography |
Important prognostic factors for disease-free survival [8].
| Favorable | |
| Initial localized disease | |
| Surgery as part of the treatment | |
| Adjuvant radiotherapy | |
| Unfavorable | |
| Age > 70 years | |
| Male sex | |
| Trunk site | |
| Head and neck site—especially lip | |
| Size of primary > 2 cm | |
| Initial nodal disease presentation, especially if >2 | |
| Initial distant disease presentation | |
| Histology—small-cell size, high mitotic rate, depth of | |
| Lymphovascular invasion | |
| Infiltrative, rather than a nodular, growth pattern |
Summary of surgical management of MCC (NCCN guidelines) [9].
| (1) Surgery is the mainstay of treatment for MCC. Radiotherapy is an inferior option for cancer control since the complete response of gross disease of MCC to radiotherapy is only 75%. | |
| (2) It is always best to perform the SLN biopsy before definitive local excision. After wide local excision, SLN biopsy may be considered in selected patients, although accuracy of results may be compromised especially in nonextremity regions. | |
| (3) Resection margin: 1-2 cm. Clear surgical margins when clinically feasible but surgeon should take into account cosmetic and functional outcomes. Close or positive margins should always be followed by adjuvant radiotherapy. | |
| (4) Different surgical techniques: local excision, wide local excision, Mohs technique, modified Mohs (Mohs technique with additional final margin for permanent section assessment), and CCPDMA (complete circumferential and peripheral deep margin assessment). | |
| (5) Any reconstruction involving extensive undermining or tissue movement is delayed until negative histological margins are verified. When primary closure is not possible, consider split-thickness skin graft as it is easier to monitor recurrence. | |
| (6) In the head and neck region, risk of false-negative SLN biopsy is higher, due to aberrant lymph node drainage and frequent presence of multiple SLN basins. SLN biopsy is therefore not mandatory. | |
| (7) SLN assessment—sensitivity of cytokeratin-20 immunohistochemical staining is over 90% and must be used. It can detect micrometastasis missed by H&E staining. |
H&E: hematoxylin and eosin; NCCN: National Comprehensive Cancer Network; SLN: sentinel lymph node.
Summary of important series of sentinel node biopsy (SLNB).
| Institute | Number of patients | Important results/conclusions |
|---|---|---|
| Helsinki University Hospital, Helsinki, Finland. Koljonen et al. [ | 15 patients | (i) False-negative lymph nodes were found in 30% of the patients. Immunohistochemical reevaluation decreased this figure to 22%. Therefore for MCC, false-negative sentinel lymph nodes can and should be limited by using immunohistochemistry. |
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| Memorial Sloan-Kettering Cancer Center, New York, United States. Fields et al. [ | 153 patients | (i) Factors associated with SLNB positivity are primary tumor size (25% ≤2 cm versus 45% >2 cm; |
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| Westmead Hospital, New South Wales, Australia. Howle and Veness [ | 16 patients, | (i) 8/16 (50%) had a positive SLN. |
CIs: confidence intervals; LVI: lymphovascular invasion; MCC: Merkel cell carcinoma; SLNB: sentinel node biopsy.
Indications for adjuvant radiotherapy; see text for more liberal indications.
| (1) Primary tumor size > 2 cm | |
| (2) Positive resection margins or tumors that closely approximate the surgical margin | |
| (3) Lymphovascular invasion in the primary tumor | |
| (4) Extracapsular extension of tumor outside nodes | |
| (5) Documented regional lymph node involvement or when regional lymph nodes were not pathologically staged |
Updated treatment algorithm for Merkel cell carcinoma [13–15].
| Stages I and II (localized disease) | |
| (i) Wide local excision with SLNB. If SLN positive, complete | |
| (ii) Wide excision and prophylactic lymph node dissection | |
| (iii) Wide excision of the primary tumor, alone or combined | |
| (iv) Mohs micrographic surgery can be used if feasible | |
| (v) Excision followed by postoperative adjuvant radiotherapy | |
| Stage III (regional disease) | |
| (i) Wide local excision plus LN dissection if feasible. If not, | |
| (ii) Adjuvant chemotherapy is controversial but may be | |
| Stage IV (distant disease) | |
| (i) Palliative care with or without surgery, radiotherapy, and |
LN: lymph node; SLN: sentinel lymph node; SLNB: sentinel lymph node biopsy.
Treatment outcomes in large series in the literature.
| Institute | Number of patients/important features | Important results/conclusions |
|---|---|---|
| Memorial Sloan-Kettering Cancer Center, New York, US. Allen et al. [ | 109 | (i) Overall DSS after recurrence was 62% |
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| Princess Margaret Hospital, Canada; Royal Prince Alfred Hospital & Westmead Hospital, Sydney, Australia. Clark et al. [ | 110 | Predictors of survival on MVA: |
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| Surveillance Epidemiology, and End Results database. Mojica et al. [ | 1665 | (i) MS for those with and without adjuvant RT: 63 versus 45 m |
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| University of Saskatchewan. Tai et al. [ | 433 | (i) Nodal metastases occurred clinically at presentation in 9/105 (9%) patients with primary tumor size 1 cm or less—too high to obviate SLNB even for small tumors |
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| Peter MacCallum Cancer Centre. Hui et al. [ | 176 | (i) Median interval to recurrence was 8 m |
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| Memorial Sloan-Kettering Cancer Center, New York, US. Fields et al. [ | 500 | (i) 50% patients died during followup: 25% died of disease, 24% died of other causes |
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| University of Bern, Switzerland. Ghadjar et al. [ | 180 | (i) RT group compared to surgery to primary tumor alone: |
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| Helsinki University Central Hospital, Norway. Kukko et al. [ | 181 | (i) No extra benefit was gained from a wide surgical margin (≥2 cm) compared to a margin of 1–1.9 cm, but an intralesional excision was more often associated with LR |
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| Memorial Sloan-Kettering Cancer Center, New York, US. Fields et al. [ | 364 | (i) 30% developed a recurrence: 3% local, 3% in-transit, 12% nodal, 12% distant |
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| Mayo Clinic, US. Grotz et al. [ | 240 | (i) 10.4% local, 7.5% in-transit, 11.3% nodal recurrences |
CI: confidence interval; DFI: disease-free interval; DFS: disease-free survival; DM: distant metastasis; DMFS: distant metastasis-free survival; DSS: disease-specific survival; LR: local recurrence; LRFS: local relapse-free survival; LRR: local-regional recurrence; LVI: lymphovascular invasion; m: months; MS: median survival; MVA: multivariate analysis; OS: overall survival; RRFS: regional relapse-free survival; RT: radiotherapy; SLNB: sentinel lymph node biopsy; s.s.: statistically significant; US: United States.