Rhabdomyosarcoma is a malignant mesenchymal tumor with features of skeletal muscle. It is the most common childhood and adolescent soft tissue sarcoma, frequently involving the head and neck in children.
Call Girls Service In Shyam Nagar Whatsapp 8445551418 Independent Escort Service
Orbital Rhabdomyosarcoma
1. Orbital Rhabdomyosarcoma
Dr Himanshu Soni
Fellow in Head & Neck Surgical Oncology – FHNO
Fellow in CMF Trauma Surgery
Oral & Maxillofacial Surgery
2. Introduction
• Tumors may arise from the musculofascial
compartment or the visceral compartment in the
head and neck region.
3. The site distribution of soft-
tissue sarcomas in the head and
neck region in adults
The distribution of soft-tissue
sarcomas in adults
4.
5. EVALUATION
• mass lesion, with or without any local pressure symptoms
• location, dimensions, consistency, and fixation to deeper structures are
important parameters to arrive at a clinical diagnosis.
Lipomas generally present with a mass that
is soft in consistency and is mobile over the
deeper soft tissues
On the other hand, hemangiomas and
lymphangiomas are also soft in consistency and
may give the impression of a compressible or
even cystic lesion.
Deep-seated and intramuscular hemangiomas
present with a diffuse ill-defined soft mass and
need radiographic assessment to define the
dimensions and location of the tumor.
tumors of fibrous tissue or neural origin present as firm to hard solid lesions.
Lesion of vasuclar origin involving the skin skin such as an angiosarcoma may have a
characteristic appearance with discoloration like ecchymosis, and nodular lesions of vascular
origin involving this skin have discoloration ranging from cherry red to purple.
6. Introduction
• Rhabdomyosarcoma (RMS) -origin is pluripotent mesenchyme
• Most common soft-tissue sarcoma of the head and neck in childhood
• Most of these tumors occur in the 1st decade of life, however RMS has
been reported from birth to the 8th decade.
7. Site of involvement
• Head and neck (including the orbit and parameningeal areas [35%]
• Genitourinary tract (including the bladder, prostate, vagina, vulva, uterus,
and paratesticular area [26%], and Extremities (19%)
• 20% of children present with disseminated disease - commonly involves
the lung
Comprises 4% of all pediatric malignancies, with 10% of all cases occurring in the orbit.
8. Etiology
• The cause of RMS is unknown; however, it is associated with several
environmental exposures including paternal cigarette use, prenatal x-ray
exposure, and maternal recreational drug use.
• In addition, RMS is the most frequently occurring childhood cancer in
families
Li-Fraumeni syndrome
neurofibromatosis type 1
Beckwith-Wiedemann syndrome
Costello syndrome.
9. Primary Ocular Rhabdomyosarcoma
1. Orbit
2. Eyelid
• Rhabdomyosarcoma confined to the eyelid is rare.
However, orbital rhabdomyosarcoma frequently presents
as a visible and palpable subcutaneous mass deep in the
eyelid. Management same as orbital
3. Conjunctival
• Rhabdomyosarcoma confined to the conjunctiva is rare.
Usually appears as a fleshy pink mass in the forniceal
conjunctiva, most often in the superior fornix
4. Anterior Uvea (Iris and Ciliary Body)
• It generally presents in an infant or young child as a
solitary, fleshy iris mass that shows slow growth.
10. Clinical features
• Proptosis developing rapidly over weeks
(80–100%)
• Globe displacement (80%) which is usually
downward and outward because two-thirds
of these tumors are supero-nasal.
11. • Locally, orbital RMS can invade the orbital bones and can extend
intracranially.
• Metastatic spread of orbital RMS is uncommon, however if left untreated
RMS has a propensity to metastasize to the lung, bone and bone marrow
mainly via hematogenous spread (because orbital lymphatics are scarce).
• Metastatic orbital RMS has an unfavorable prognosis when compared to
localized disease
12.
13. World Health Organization
Four variants of rhabdomyosarcoma
Embryonal (65%)
Alveolar (25%)
Pleomorphic
Spindle cell/sclerosing rhabdomyosarcoma
14. TYPES OF RMS:
1.Embryonal rhabdomyosarcoma:
• Embryonal rhabdomyosarcoma (ERMS) is the
most common histological variant, comprising
approximately 60-70% of childhood cases
• ERMS is characterized by spindle-shaped cells
with a stromal-rich appearance
• ERMS also has two defined subtypes, boytroid
and spindle cell ERMS, and these subtypes are
associated with a favorable prognosis
Rhabdomyosarcoma can be generally divided into three histological subsets
15. 2.Alveolar rhabdomyosarcoma:
• It is the second most common type. ARMS
comprises approximately 20-25% of RMS-
related tumors, and it is equally distributed
among all age groups.
• most common form of RMS observed in young
adults and teenagers, who are less prone to the
embryonal variant.
• This type of RMS is characterized by densely-
packed, round cells that arrange around spaces
similar in shape to pulmonary alveoli.
• It is also typically more aggressive than ERMS.
16. 3.Anaplastic rhabdomyosarcoma:
• Anaplastic rhabdomyosarcoma is defined by the presence of anaplastic
cells with large, lobate hyperchromatic nuclei and multipolar mitotic
figures
• The anaplastic cells may be diffuse or localized, with the diffuse variation
correlating to a worse prognosis. It occurs most often in adults, rarely in
children
17. BOTRYOID TYPE
• Subtype of Embryonal
• 10% of all Childhood RMS
• Mucosal Surface
Vagina
Billiary
Bladder
Nasopharynx
• Most common in hollow visceral organs - GU
tract
• Superior Prognosis
Polypoid, grape-like tumor masses,
Scattered malignant cells in myxoid
stroma
19. Locations
• Defined as parameningeal (50%), nonparameningeal (25%), and
orbital (25%).
• Parameningeal tumors, which include the nasopharynx, paranasal
sinuses, middle ear, mastoid, and infratemporal fossa, have the
worst prognosis because of their proximity to vital structures.
• Orbital and nonparameningeal tumors have an excellent prognosis.
20. Head & Neck (Para-meningeal)
• Sites: Nasopharynx, Nasal cavity, PNS, Middle ear, Pterygopalatine fossa.
• Have propensity for base skull invasion & intracranial extension.
• Common histological subtype: ERMS.
• Incidence of lymph node involvement (IRS III): <20%.
• Possibility of complete surgical excision (IRS III): <25%.
21. Head & Neck ((Non-parammeningeal)
• Sites: Parotid, Oral cavity, Oropharynx and Larynx.
• Common histological subtype: Embryonal RMS.
• Buccal mucosa: Alveolar RMS
• Incidence of lymph node involvement (IRS III) <20%.
• Prophylactic / Elective nodal irradiation not recommended
22. Diagnosis
What to ask ????
• detailed history is essential in any child suspected to have orbital RMS (i.e.
under 2 years of age and presenting with an orbital mass).
• Pain
• visual loss
• signs of sinusitis
should also keep in mind possible misleading presentations such as rapidly
progressing
• alterations of the lid, conjunctiva or caruncle.
23. Imaging
• In early stages the tumor is well circumscribed, but in later stages, where
there is pseudocapsular invasion, the borders are irregular. There may be
some bone deformity, but frank bone destruction with bone involvement is
rare, and the diagnosis in this case will change from orbital to
parameningeal RMS. The tumor may show hemorrhages and cyst
formation.
Orbital RMS is usually extraconal (37–87%) or both intra and extraconal (13–
47%), and more commonly superonasal in location especially for embryonal
RMS (inferior location is more common for alveolar).
24. • CT and MRI are the modalities of choice for assessment of these masses, and to
delineate adjacent structures.
• It is important to report the location of the tumor epicenter as there is a correlation
between location and histology: embryonal subtype more frequently arises in the
superior orbit, whereas alveolar subtype is more common in the interior orbit
25. CT
• Orbital RMS appears as a well-circumscribed, homogenous, soft tissue mass
that is isodense as compared to muscles without bone destruction in earlier
stages, but with invasion of surrounding structures and calcification in more
advanced cases where there is destruction of the adjacent bone.
• A heterogeneous appearance is possible in the event of focal hemorrhage or
necrosis, and there is moderate to marked general enhancement with
intravenous contrast.
• A common finding is eyelid thickening, regardless of lid involvement, and a
less common finding is a cavitated mass with ring-like enhancement.
• When using CT one must be aware that exposure to ionizing radiation may
theoretically induce a second potentially fatal cancer in children who have
already manifested a tendency to harbor cancer.
26. MRI
• T1
▫ low to intermediate intensity, isointense to adjacent muscle
▫ areas of hemorrhage are common in alveolar and pleomorphic subtypes, but
these are uncommon in the orbit 1
• T2
▫ usually hyperintense
• T1 C+ (Gd): shows considerable enhancement
27. • Diffusion-weighted imaging (DWI) is an MR imaging technique that gives
information about normality of proton and water diffusion through tissue
characterized by DWI and ADC (Apparent Diffusion Coefficient) values,
respectively.
• Because of high cellular density, malignant tumors usually have restricted
diffusion.
• They found that RMS was predominantly restricted on DWI/ADC, which was
especially helpful in differentiating it from hemangioma, (which has increased
DWI/ADC) since the two exhibit a similar appearance on T1 and T2.
28. Ultrasound
• It mainly appears as a well-circumscribed, heterogenous, irregular mass
with low to medium echogenicity on US and a variable intratumoral
vascular flow pattern on Doppler US.
• A ‘‘pseudocystic’’ appearance has been reported as characteristic, and that
is thought to be due to spindle cells in embryonal RMS which have
abundant cytoplasm and are separated loosely by edematous fluid.
29. Biopsy
• RMS is the most common biopsied malignant orbital tumor in a child, and it is
important in terms of establishing diagnosis and determining prognosis.
• The biopsy can be incisional or excisional based on clinical and imaging
findings, however fine needle aspiration is less useful because the limited
amount of tissue obtained is usually insufficient for pathological diagnosis.
• Its is advised incisional biopsy, as opposed to excisional, in order to avoid
dissemination of tumor cells into the adjacent healthy tissue.
30. Immunohistochemistry
• Immunohistochemical studies constitute the main approach to diagnosis.
The markers typically found in RMS include antibodies against desmin
(90%), muscle-specific actin, myoD1 (71–91%) and myoglobin.
• Myogenin (90%) is expressed more in the alveolar than in the embryonal
type.
• Vimentin and desmin are usually positive but less specific since they can
be positive in other tumors with skeletal muscle differentiation.
• Myogenin and MyoD1 are myogenic transcriptional regulators that are
expressed early in skeletal muscle differentiation (earlier than desmin,
actin, myoglobin and myosin).
31. Guidelines regarding management of RMS since the
early seventies have been intoduced mostly by the -
• Prior to that, overall survival (OS) was about 25–30% (with the historically
recommended treatment being exenteration prior to the late 1960’s), and
with the introduction of surgery combined with adjuvant chemotherapy as
well as radiotherapy in cooperative group trials OS improved to around
90%.
North American Intergroup Rhabdomyosarcoma Study Group (IRSG)
European cooperative groups: International Society of Pediatric Oncology-Malignant
Mesenchymal Tumor Tumor Committee (SIOP-MMT),
Cooperative Weichteilsarkom Study Group (CWS)
Italian Cooperative Group (ICG).
32. Management
• Group I: localized disease, completely resected (excisional
• biopsy).
• Group II: microscopic disease remaining after biopsy.
• Group III: gross residual disease remaining after biopsy.
• Group IV: distant metastasis present at onset.
Following biopsy, staging for orbital RMS is internationally uniformly done according
to the IRS post-surgical staging system.
This classification is useful in terms of treatment, stratification
and prognosis prediction.
35. Current management includes surgery, irradiation and
chemotherapy depending on the stage.
• Group I are treated with chemotherapy only: VA (vincristine and actinomycin).
• Group II are treated with a combination of chemotherapy (VA and
cyclophosphamide; VAC) and radiotherapy (36 Gy).
• Group III are treated with a combination of chemotherapy (VAC) and radiotherapy
(45 Gy).
• Group IV are treated with a combination of intensive chemotherapy and
radiotherapy.
36. The current European Soft tissue sarcoma Study
Group (EpSSG) protocol (EpSSG-RMS-2005) proposes the
following treatment strategy
• Group I: chemotherapy consisting of VA.
• Groups II and III: chemotherapy VA with Ifosfamide added in the first four courses;
when in complete remission after three chemotherapy courses policy is to either
leave out radiotherapy but add more ifosfamide, or add radiotherapy (36 Gy) and
leave out further ifosfamide. Those not in complete remission after induction
chemotherapy get radiotherapy (45 Gy) without further ifosfamide.
• Group IV: intensified chemotherapy regimen (IVA and doxorubicin) followed by
one year of maintenance chemotherapy and radiotherapy to all involved sites (when
possible).
37.
38. AMORE protocol
• For the treatment of non resectable head and neck RMS.
• This protocol has since been followed for orbital RMS with the only
remark that reconstruction is often not needed at the orbital site.
It consists of Ablative surgery,
MOulage technique brachytherapy
surgical REconstruction;
• it targets residual tumor mass.
39. Brachytherapy has advantages over EBRT
• Reduction in the treatment time
• Focused dose delivery to the tumor bed and rapid fall-off of the dose beyond the treatment
volume, this way
• Sparing surrounding tissues and reducing morbidity,
• Allowing organ preservation and bone growth,
• Potentially improving the functional and cosmetic outcome.
AIM of PROTOCOL -
•maximize local treatment and to avoid external beam radiotherapy (EBRT).
•Ablative surgery is performed as conservatively as possible with an effort not to
sacrifice important tissue at the expense of possible microscopic remnants- which will
be amenable to the brachytherapy which is initiate directly post surgery.
40. Radiotherapy
• Radiation is usually in the range of 3600–5040 cGy over 4– 5 weeks, and in
the case of parameningeal extension the region of extension is irradiated + 2
cm.
• The main goal in novel management options is to maintain excellent survival
while reducing the late side effects of treatment.
• All of this has prompted enthusiasm for no or reduced- dose radiotherapy in
low-risk RMS and for new technologies in radiation oncology including
proton beam radiotherapy, intensity modulated radiotherapy (IMRT), 3-D
conformational radiotherapy and implant brachytherapy all with the goal to
minimize dose to normal tissue.
41. IMRT
• Hein et al. focused on the possibility of organ-sparing (particularly lens-
sparing) irradiation in children with orbital RMS by using IMRT as opposed
to 3D conformational photon radiotherapy.
• They concluded that although IMRT resulted in a reduced dose to the lens (in
treating tumors in retrobulbar and lateral positions) and ipsilateral lacrimal
gland, no significant difference was noted for the ipsilateral retina and optic
nerve, and more importantly, it resulted in an expanded volume of the brain
receiving low dose radiation as compared to 3D conformational radiotherapy.
Oberlin O, Rey A, Lyden E, Bisogno G, Stevens MC, Meyer WH, et al. Prognostic factors in metastatic rhabdomyosarcomas: results of
a pooled analysis from United States and European cooperative groups. J Clin Oncol 2008;26:2384–9.
42. Fractionated proton radiotherapy
• Yock et al. reported results on using fractionated proton radiotherapy as
superior over 3D conformational photo radiotherapy for orbital RMS; they
concluded that proton therapy achieves excellent tumor coverage at the
same time as it reduces radiation to the adjacent normal tissue like the
brain, pituitary, hypothalamus, temporal lobes, and ipsilateral and
contralateral orbital structures.
• Proton irradiation has excellent potential for conformal treatment to
normal tissue that is better than 3D conformal radiation and perhaps even
IMRT- which although advanced in tumor targeting as compared to 3D
conformational photon irradiation- does distribute low dose to normal
tissue: a disadvantage in a pediatric population with excellent survival that
is more prone to secondary malignancies and growth retardation.
44. Brachytherapy
• Brachytherapy offers a high dose to the tumor bed with a low dose to the
surrounding tissues and can be considered in cases where radiotherapy
is necessary and brachytherapy characteristics fit; and although there are
no conclusive clinical data available yet, the findings after IMRT might
seem to be less favorable than those of brachytherapy.
• Following SIOP guidelines, Blank et al. have recently reported the use of
brachytherapy instead of EBRT as part of the treatment of orbital RMS.
• The side effects were found to be very low and not clinically significant.
They thus concluded that surgery followed by brachytherapy can be
considered when there is no residual intracranial extension of the tumor
after chemotherapy, macroscopic tumor removal is feasible, and when
EBRT is expected to be harmful to eye structures.
45. • Doses for node-negative microscopic residual disease are 36 Gy
• 41.4 Gy for those with microscopic disease and pathologically proven but
grossly negative nodal disease.
• For a gross residual tumor, the recommended dose is 45 Gy for orbital and
50.4 Gy for nonorbital primary sites
46. • Selection of reduced doses of radiation for
patients with orbital sites of involvement is
supported by the D9602 trial
47. • The treatment volumes for patients requiring
radiation include
• – All areas of gross disease
• – Areas the tumor initially infiltrated at
diagnosis
• The timing of radiation therapy usually occurs
after the initial 12 or 18 weeks of chemotherapy
48. Systemic Therapy
• Most common regimen used in North America
consists of vincristine, actinomycin D, and
cyclophosphamide (VAC)
• Ifosfamide is preferentially used in the European
trials
49.
50. Conclusion
• Orbital RMS is one of the few life-threatening diseases that present first to
the ophthalmologist; therefore prompt diagnosis and treatment is a life-
saving issue.
• Hence, knowledge of the clinical, histopathological, and radiographic
features as well as the more recent advances in the management of this
entity is essential.
Masses on the face, neck, or scalp show a visual deformity, and those in the oral cavity, pharynx, or larynx may have symptoms of obstruction to the upper aerodigestive tract.
Rhabdomyosarcoma is a malignant mesenchymal tumor with features of skeletal muscle [8]. It is the most common childhood and adolescent soft tissue sarcoma, frequently involving the head and neck in children [44].
RMS is also associated with disorders in development, including central nervous system, genitourinary, gastrointestinal, and cardiovascular anomalies, and with congenital disorders including congenital pulmonary cysts, Gorlin basal cell nevus syndrome, and neurofibromatosis.
The most common mode of presentation is a mass lesion or symptoms resulting from pressure on contiguous neurovascular structures or the viscera
Pleomorphic rhabdomyosarcoma is primarily a tumor of older adults,
rare spindle cell–sclerosing subtype, which was added by WHO in 2013, occurs in both children and adults.
Approximately 40% of rhabdomyosarcomas involve the head and neck
Patients typically present with a painful or painless mass causing symptoms related to mass effect.
Metastatic disease is present in 15% of patients at initial presentation
An increased incidence of rhabdomyosarcoma has been reported in patients with neurofibromatosis type 1 (NF1)
On MRI, the tumor appears isointense with respect to extraocular muscles and hypointense with respect to orbital fat on T1-weighted images, and hyperintense (with respect to both orbital fat and extraocular muscles) on T2-weighted image.
Diffusion-weighted imaging (DWI) is a form of MR imaging based upon measuring the random Brownian motion of water molecules within a voxel of tissue. In general simplified terms, highly cellular tissues or those with cellular swelling exhibit lower diffusion coefficients.
Apparent diffusion coefficient (ADC) is a measure of the magnitude of diffusion (of water molecules) within tissue, and is commonly clinically calculated using MRI with diffusion-weighted imaging (DWI)
Decision-making for management is based on histopathologic
confirmation as well as staging of orbital RMS, which is
done by reviewing imaging (MRI of primary tumor, chest-CT,
Tc bone scan), pathology, and further work-up for metastases
(bilateral bone marrow punctures and trephines).
After diagnosis and staging, chemotherapy is given according to the European protocol, after which imaging is repeated to look for residual disease.
Wolden et al. studied IMRT for head-and-neck RMS where
they used a smaller margin (1.5 cm as opposed to the standard
2 cm in IRSG protocols) made possible by using imaging
(CT, PET, MR) in radiotherapy planning.59 They concluded
that IMRT with image fusion achieved excellent local control
(in cases that did not have alveolar histology) with minimal
dose reaching adjacent tissue when dose-limiting structures
are adjacent to the tumor.
Reduced doses of radiotherapy without an alkylating agent in patients with embryonal group IIA and orbital group III tumors did not compromise local control rates (~15% local failure).
Cyclophosphamide and ifosfamide can damage the bladder, causing blood in the urine. The risk of this happening can be lowered by giving the drugs with plenty of fluids and with a drug called mesna, which helps protect the bladder.
Vincristine can damage nerves. Some patients may notice tingling and numbness (called neuropathy), particularly in the hands and feet. This often goes away or gets better once treatment is stopped, but it could last a long time in some people.