Key Points

Incidence

Annually, there are 350 cases of pediatric rhabdomyosarcoma (RMS) in the United States. Of those, embryonal rhabdomyosarcoma (ERMS) comprises 75% (260 cases), and alveolar rhabdomyosarcoma (ARMS) comprises 25% (90 cases). Annually, there are 500 cases of pediatric non-rhabdomyosarcoma soft-tissue sarcoma (NR-STS) in the United States. These are divided into high-grade (Pediatric Oncology Group [POG] grade III), 67% (335 cases), and low and intermediate grade (POG grade I/II), 33% (165 cases).

Biologic Characteristics

RMS: ERMS often demonstrate loss of heterozygosity of 11p15 and a higher rate of somatic mutations than ARMS. Recurrent mutations in the RAS pathway are observed; ERMS with anaplastic features may harbor germline TP53 mutations. Of ARMS, 80% harbor translocations of FOXO1 with either PAX3 (t(2;13)(q35;q14) or PAX7 (t(1;13)(p36;q14). There are diverse histologies in NRSTS, with a mixture of distinct genetic events. Examples include: Synovial cell sarcoma: t(X;18) and resulting fusion product SYT-SSX ; Alveolar soft-part sarcoma: der(17)t(X;17) and resulting fusion TFE3-ASPL ; Epithelioid sarcoma: SMARCB1 mutations.

Staging Evaluation

RMS: Risk stratification has utilized pretreatment TNM staging classification (including tumor size, location, and invasiveness) as well as clinical grouping (Intergroup Rhabdomyosarcoma Study Group (IRSG)) based on degree of surgery, nodal involvement, and metastatic disease. Current and future clinical trials will incorporate fusion protein status for risk classification. NR-STS uses the American Joint Committee on Cancer staging system, which is based on grade, size, invasiveness, nodal involvement, and metastatic disease.

Primary Therapy

For RMS, nonmorbid “upfront” surgery is the first line of therapy. Radiotherapy (RT) is used for primary and metastatic sites of disease. The following are recommended doses: Microscopic disease: 36 Gy; microscopic nodal disease: 41.4 Gy; and gross disease: 50.4 Gy. Local failure rates are 10% for Group I/II and 13% for Group III. For NR-STS, the recommended course is surgical resection with or witshout adjuvant RT (55.8 Gy to 63 Gy) or brachytherapy (34 Gy at 3.4 Gy twice daily, high-dose rate). For initially nonresectable tumors, preoperative chemoradiation (conventionally fractionated external beam RT, 45 Gy to 50.4 Gy) followed by surgery is needed. Local failure rates are 4% for completely resected and range from 40% to 80% for nonresected disease.

Adjuvant Therapy

For RMS, vincristine, dactinomycin (Actinomycin D), cyclophosphamide (VAC)–based chemotherapy is the standard. For high-risk disease, vincristine, irinotecan, dactinomycin, cyclophosphamide, doxorubicin, ifosfamide, etoposide, or experimental agent(s) is used. With these treatments, there is a 5-year event-free survival: Low risk (group I/II embryonal RMS): 90%; Intermediate risk (ARMS groups I-III, ERMS group III): 70% to 73%; and high risk (metastatic embryonal or alveolar RMS): less than 30%. In NR-STS, neoadjuvant chemoradiation or adjuvant chemotherapy (ifosfamide/doxorubicin) is used. There is a 5-year event-free survival: Localized, resected: 75%; localized, nonresectable: 45%; and metastatic: 10%.

Epidemiology

Soft-tissue sarcomas (STS) account for approximately 7% of all pediatric cancers. RMS comprises 40% of STS, and the other NR-STS comprise 60%. This results in 350 patients with RMS and 500 with NR-STS (divided about 2 : 1 between high and low grade) available for participation in clinical trials in the United States annually. Based on prior clinical trials, 75% of children with RMS require RT; based on the presence of high-grade disease only, approximately two-thirds of children with NR-STS receive irradiation. This yields 600 sarcoma cases annually for the study of radiation-specific clinical trial questions, training of young radiation oncologists, and study of radiation-specific long-term sequelae.

Patients with RMS have benefited from the Children's Oncology Group (COG) sarcoma studies (formerly the IRSG). The trials conducted by these groups have defined the combined modality treatment of children with RMS in North America and allowed the randomized comparisons of new chemotherapeutics as well as RT strategies that would not be possible without the cooperative group structure. These approaches, as well as the specifics of modern RT, are discussed in this chapter.

Treatment of children with NR-STS is less well defined. Local therapy approaches have evolved from adult paradigms, incorporating limb salvage over amputation, adjuvant irradiation, and subsequently, preoperative RT approaches. Despite adult parallels to draw from, little prospective research has been conducted in the pediatric NR-STS population. A recent COG prospective clinical trial (ARST0332) sought to address some of these deficiencies by defining risk groups based on histologic grade, tumor size, resectability, and presence of metastases; preoperative and postoperative RT are delivered in conjunction with surgery and chemotherapy to define the role of local and systemic approaches among risk groups. Preliminary data from this study suggest that a risk-based approach may allow for RT dose limitation or exclusion in select patients.

Biologic Characteristics and Pathology

Rhabdomyosarcoma

Rhabdomyosarcoma is broadly classified as one of the small, round, blue cell malignancies of childhood. The 2013 World Health Organization (WHO) classification of RMS includes several histologic subtypes: ERMS, the most common form (with botryoid comprising a favorable variant); spindle cell/sclerosing RMS; ARMS; and pleomorphic RMS. Pleomorphic RMS is typically seen in adults and is considered to have poor prognosis. Light microscopy often describes ERMS with spindle-shaped cells and ARMS with small, round, blue cells forming alveolar-like spaces, although tumor biopsy specimens may also look like collections of poorly differentiated cells complicating definitive diagnosis by hematoxylin and eosin staining alone. Cytogenetic events occur in ERMS with a loss of heterozygosity on chromosome 11p15 and frequent mutations of the RAS/NF1 pathway. Anaplastic features in ERMS may indicate a possible germline TP53 mutation and diagnosis of Li-Fraumeni syndrome ; 80% of ARMS harbor translocations between FOXO1 on chromosome 13 and loci of either PAX3 ((t(2;13)(q35;q14)) or PAX7 (PAX7 (t(1;13)(p36;q14)). The resultant fusion proteins from these translocations act as transcription factors; fusion-positive tumors are considered biologically and clinically distinct from fusion-negative ARMS. Congenital/infantile spindle cell RMS have demonstrated fusions commonly involving VGLL2 , whereas sclerosing RMS often have MYOD1 mutations, occasionally concomitant with activating mutations of PIK3CA . Other genetic predisposition syndromes associated with RMS include neurofibromatosis type 1 (with a prevalence of 1 : 200 noted on IRSG-IV), pleuropulmonary blastoma/ DICER1 syndrome (typically genitourinary ERMS), Costello syndrome ( HRAS mutations), Noonan syndrome, and Beckwith-Wiedemann syndrome.

Nonrhabdomyosarcoma Soft-Tissue Sarcoma

The pediatric NR-STS comprise a heterogeneous group of tumors managed homogeneously largely because of the limitations in patient numbers and effective chemotherapy. The most common histologies include synovial cell sarcoma and malignant peripheral nerve sheath tumor, although several rarer variants, including infantile fibrosarcoma, are almost exclusive to the pediatric age group. Although many NR-STSs have no genetic signature, several histologic variants do have specific translocations or deletions ( Table 79.1 ). Others may harbor specific recurrent mutations, such as SMARCB1 aberrations seen in epithelioid sarcoma.

TABLE 79.1
Genetic Abnormalities: Nonrhabdomyosarcoma Soft-Tissue Sarcomas
Histology Genetic Abnormality
Synovial cell sarcoma t(X;18); fusion SYT-SSX
Clear-cell sarcoma t(12;22); fusion EWS-ATF1
Desmoplastic small round cell tumor t(11;22); fusion EWS-WT1
Infantile fibrosarcoma t(12;15); fusion ETV6-NTRK3
Alveolar soft-part sarcoma der(17)t(X;17); fusion TFE3-ASPL
Low-grade fibromyxoid sarcoma t(7;16); fusion FUS-CREB3L2
Myxoid and round cell liposarcoma t(12;16); fusion FUS-DDIT3

Clinical Manifestations

Rhabdomyosarcoma

The presentation of children with RMS is diverse, characterized by the site of involvement and extent of disease. The median age for children presenting with RMS is younger than 5, although a second incidence peak occurs in the mid-teens. The head and neck region is the most frequent site of involvement and is divided into favorable and unfavorable (parameningeal) sites. Other common sites include the genitourinary tract (with bladder and prostate less favorable) and extremities. Trunk, chest wall, perineal, retroperitoneal, and biliary tree primary tumors are seen less frequently. Metastatic disease occurs 20% of the time at presentation, and nodal involvement is rare (< 5%) except for paratesticular (25%) and extremity (24%) sites of disease, which warrant computed tomography (CT) including paratesticular sites at younger than 10 years of age), nodal sampling (paratesticular sites for10 years of age or older), or sentinel node biopsy (extremity sites).

Nonrhabdomyosarcoma Soft-Tissue Sarcoma

The presentation of NR-STS is often as a painless mass; additional symptoms may be site specific. Approximately 50% of cases arise in an extremity, and incidence increases throughout the adolescent years and into adulthood. Although many patients suspected to have soft-tissue “masses” are identified to have either normal tissues or a benign lesion, consideration should always be given to malignancy because an ill-chosen surgical approach may compromise future local therapy ( Fig. 79.1 ).

Fig. 79.1, Rhabdomyosarcoma of the Pinna of the Ear Presenting as a Painless Soft-Tissue Mass.

Of patients, 15% to 20% present with metastatic disease at diagnosis, with the lungs being the predominant site of metastatic involvement. Clear-cell sarcoma and epithelioid sarcoma carry a risk of regional nodal involvement and warrant evaluation of the draining nodal bed(s) with sentinel node sampling.

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