Soft tissue lesions strike fear in many pathologists as they are uncommon and may be difficult to diagnose.

Introduction

WHO classification of soft tissue lesions/tumours

Morphologic grouping^[1]

1. Adipocytic tumours.
2. Fibroblastic/myofibroblastic tumours.
3. "Fibrohistiocytic" tumours.
4. Smooth muscle tumours.
5. Skeletal muscle tumours.
6. Vascular tumours.
7. Perivascular (pericytic) tumours.
8. Chondro-osseous tumours.
9. Tumours of uncertain differentiation.

Biologic potential grouping^[2]

1. Benign.
2. Intermediate (locally aggressive).
3. Intermediate (rarely metastasizing).
4. Malignant.

Prevalence

• All sarcomas are rare buggers.
  • As the classification has been changing over the past years (with more subtypes being recognized/identified) numbers are variable from study-to-study.
• Once upon a time almost everything was called malignant fibrous histiocytoma; thus, it is listed as a common entity in some publications.

Most common:^[3]

• Liposarcoma.
• Leiomyosarcoma.

Molecular testing

• Molecular testing plays an important role in soft tissue pathology.
• It is generally seen as an adjunct test that:^[4]
  • Often is used to confirm the histomorphologic impression/quality control.
  • Frequently has some prognostic significance.
  • May directly affect treatment.

Translocations

• Many tumours in soft tissue pathology are diagnosed inconjunction with the finding of chromosomal translocations.

Histologic patterns

Grading

• Several systems exist.
• The US-CAP advocates the use of the French system over the NCI system.
  • The French system is a better predictor metastases and mortality.^[7]

French system

Overview:^[7][8]

1. Differentiation (score 1-3).
   • De facto, this is mostly the histologic type.
2. Mitotic rate (score 1-3).
3. Necrosis (score 0-2)

Obtaining a score:

• Add all the points from the three components.

Scoring:

• Grade 1 = 2-3.
• Grade 2 = 4-5.
• Grade 3 = 6-8.

Differentiation

• Standardized for histologic types.
• Most tumours = 3/3.

Exceptions:^[8]

• Well-differentiated liposarcoma = 1.
• Myxoid liposarcoma = 2.
• Conventional liposarcoma = 2.
• Fibrosarcoma = 2.
• Myxofibrosarcoma =2.

A group of tumours is not graded:^[8]

• MPNST.
• Rhabdomyosarcoma.
• Alveolar soft part sarcoma.
• Clear cell sarcoma.
• Extraskeletal myxoid chondrosarcoma.

Mitotic rate

• 0-9 mitoses/10 HPF.
• 10-19 mitoses/10 HPF.
• >=20 mitoses/10 HPF.

Notes:

• 1 HPF = 0.1734 mm^2.
  • Most resident microscopes have a field of view = 0.2376 mm^2.
    • Thus, ~7.3 HPFs on a resident microscope corresponds to 10 US-CAP HPFs.

Necrosis

• None = score 0.
• <=50% of tumour = score 1.
• >50% of tumour = score 2.

System used by some at MSH

Some pathologists at MSH use the system advocated by Costa et al..^[9]

Scoring

• Grade 1 = 1 point.
• Grade 2 = 2 points.
• Grade 3 = 3-4 points.

Components

Points for each of the following:

• Mitotic activity >= 6 / 10 HPF @ 40X - definition suffers from HPFitis.
• Pleomorphism present.
• Cellularity (cells/matrix) > 50%.
• Necrosis >15% - microscopic (without targeting necrosis grossly) or grossly.

Adipocytic tumours

This category includes:

• Lipoma.
• Liposarcoma.
• Hibernoma.

Smooth muscle tumours

Leiomyosarcoma

Microscopy

Features:

• Nuclear atypia.
• Necrosis.
• Mitoses.

Fibrohistiocytic tumours

Pleomorphic undifferentiated sarcoma

• Abbreviated PUS.
• AKA Undifferentiated pleomorphic sarcoma.
• Previously known as malignant fibrous histiocytoma, abbreviated MFH.^[10]

General

• Common sarcoma.
• Usu. deep tissue of the trunk and extremities.

Microscopic

Features:^[11]

• Storiform pattern (AKA patternless pattern) - key feature.
• Marked nuclear pleomorphism key feature.
  • Variation is nuclear size, nuclear shape and nuclear staining (esp. hyperchromasia).
• Mitoses - abundant; atypical mitoses common.
• Necrosis (common).
• Mix of spindle cells and epithelioid cells.

Other findings:

• +/-Giant cells (see subclassification).
• +/-Inflammation (see subclassification).
  • Neutrophils.
  • Eosinophils.

Image:

• PUS - high mag. (WC).
• PUS - intermed. mag. (WC).

Subclassification

Pleomorphic sarcoma (PS) is subclassified the following way:^[12]

• PS with giant cells.
• PS with inflammation.
• PUS (not otherwise specified) - wastebasket diagnosis; if neither of the above two apply.

Fibroblastic/myofibroblastic tumours

Nodular fasciitis

General

• Benign.
• All age groups.
• Associated with trauma.

Microscopic

Features:^[13][14]

• Usu. well-circumscribed.
• Clusters of (non-pleomorphic) spindle cells.
• Inflammation (lymphocytes).
• Microcysts in cellular regions - uncommon - discriminatory.
• Mitoses - common.
• Extravasated RBCs.

The BD feature list:^[15]

• Tissue culture-like/CNS-like morphology.
• Thick (keloid-like) collagen bundles - key feature.
• Extravasated RBCs.
• Inflammation.
• +/-Giant cells.

Notes:

• No significant nuclear atypia.
• No atypical mitoses.
• May be cellular.

Images:

• NF - low mag. (WC).
• NF - high mag. (WC).

IHC

Routine spindle cell panel:

• CD34 -ve.
• Desmin -ve..
• SMA -ve.
• S100 -ve.
• AE1/AE3 -ve.

Others:

• H-caldesmon -ve.
• EMA -ve.
• Vimentin +ve.

Molecular

• Evolving - case reports.
  • t(15;15)(q13;q25).^[16]

Desmoid-type fibromatosis

• AKA desmoid tumour.

General

• Benign.
• Locally aggressive.^[17]
• May be seen in the context of familial adenomatous polyposis.

Microscopic

Features:^[18]

• Abundant fibroblasts.
  • Arranged in bundles or fascicles.
• +/-Collagen.

IHC

Features:^[18]

• Beta-catenin +ve.
• SMA +ve ~50% of lesions.

Proliferative fasciitis

• Need to write something here.

Solitary fibrous tumour

General

• Grouped with hemangiopericytoma in the WHO classification; possibly the same tumour (?).^[18]
• May be benign or malignant; more commonly benign.^[19][20]

Microscopic

Features:

• Well-circumscribed.
• Fibroblast-like cells (spindle cells).
• Hemangiopericytoma-like area (staghorn vessels) - not seen on image.
• Keloid-like collagen bundles.

Images:

• SFT - low mag. (WC).
• SFT - intermed. mag. (WC).
• SFT - high mag. (WC).

IHC

• CD34 ~90% +ve.
• CD99 ~70% +ve.
• BCL2 ~50% +ve.

Hemangiopericytoma

General

• Grouped with solitary fibrous tumour in the WHO classification; possibly the same tumour (?).^[18]
• Arises from the pericyte, a connective tissue cell of small vessels that is thought to be involved in flow regulation.
• Hematologic spread most common - to lungs.^[21]
• Oncogenic osteomalacia - assoc. with hemangiopericytoma.^[22]

Presentation

• Usually painless mass, slow enlargement.

Radiology

• Intramedullary lytic mass.
• May be well-circumscribed.
• +/-Periosteal reaction.
• +/-Sclerotic border.

May be worked-up with angiography to distinguish from a vascular malformation.^[23]

Location

• Usually extremities - femur or prox. tibial.^[24]

Histology

Features:^[25]

• Hypervascular lesion - key diagnostic feature.^[26]
  • Abundant thin-walled branching small vessels of variable size.
    • May be described as "staghorn vessels" or "antler-like" vasculature.
    • Cells may "onion-skin" around thin blood vessels.
• Spindle or ovoid shaped cells in nests or sheets.

IHC

Features:^[18][26]

• Vimentin +ve (usually).
• Desmin -ve (typical).
• Factor VIII -ve (marks endothelium).
• CD34 +ve.
  • CD34 usu. -ve in synovial sarcoma.
• CD31 -ve (marks benign endothelium).
• vWF (von Willebrand factor) -ve.

May be in the DDx for meningioma:^[27]

• EMA -ve.
• S100 -ve.

DDx

• Other vascular tumours.
• Vascular malformations.
• Synovial sarcoma.

Desmoplastic fibroblastoma

• AKA collagenous fibroma.^[28]
• Benign lesion.
• Classically found in shoulder region.

IHC

• Beta-catenin -ve.^[29]
  • Significance ???

Low-grade fibromyxoid sarcoma

• AKA hyalinizing spindle cell tumour.

General

• Deep soft tissue.

Microscopic

Features:^[30]

• Myoid stroma - key feature.
• Low cellularity.
• Spindle cells.

Notes:

• Few/absent mitoses.

Molecular pathology

t(7;16)(q33;p11)^[31]

Perivascular tumours

This grouping includes only two:^[32]

• Glomus tumour - both benign and malignant.
• Myopericytoma.

Vascular lesions

Vascular lesions are "too red"; they have too many RBCs.

They include:

• Hemangioma.
• Kaposi sarcoma.
• Masson hemangioma.
• Angiosarcoma
• Epithelioid hemangioendothelioma.

Skeletal muscle tumours

Rhabdomyoma

Rhabdomyosarcoma

• Abbreviated RMS.

Comes it two main flavours:

• Alveolar rhabdomyosarcoma.
• Embryonal rhabdomyosarcoma.

The histology may be that of a small round cell tumour.

Chondro-osseous tumours

This grouping includes tumours derived from cartilage and bone.

Tumours of uncertain differentiation

Ewing sarcoma/PNET

• A small round blue cell tumour that may be seen in bone. It is discussed in the context of bone tumours.

Epithelioid sarcoma

General

• Rare.
• Adolescents, young adults.

Microscopic

Features:^[33]

• Epithelioid morphology and spindle morphology.
• Prominent nucleolus - key feature.
• Zonal necrosis with irregular border.
  • Descriptors: "Garland necrosis", necrosis with "scalloped border" = necrotic regions with irregular border.

DDx:

• Rheumatoid nodule.
• Granuloma annulare.

Microscopic

Features:^[34]

• INI1 (SMARCB1^[35]) -ve.^[36]
• Vimentin +ve.
• Various keratins +ve.
  • Keratin 8, Keratin 19 +ve.
  • 34betaE12 +ve/-ve.
• CD34 +ve.
  • Malignant rhabdoid tumour -ve.

Others:

• S100 -ve (r/o melanoma).

Alveolar soft part sarcoma

• Abbreviated ASPS.

General

• Adolescents/young adults.
• Children -- classically location: base of tongue and orbit.

Microscopic

Features:^[37]

• Arranged in nest/separated by thin septa; vaguely resembles alveoli (at low power).
• Large cells (~30-50 μm) with abundant eosinophilic cytoplasm.
• An eccentric nucleus.
• +/-Nucleolus.

Images:

• ASPS - low mag. (WC).
• ASPS - intermed. mag. (WC).
• ASPS - very high mag. (WC).

Molecular

• t(X;17)(p11.2;q25).^[38]

Desmoplastic small round cell tumour

• Abbreviated DSRCT.

General

• Males > females.
• Usu. affects young adults.
• Typically retroperitoneal.
• Poor prognosis.

Microscopic

Features:^[39]

1. Broad bands of paucicellular fibrous stroma with:
2. Small round cells in nests with an undulating sharp border.
   • The small round cells lack distinct nucleoli and have scant cytoplasm; they are small round cell tumour cells.

Notes:

• Usu. abundant mitoses.
• +/-Necrosis.

Images:

• DSRCT - intermed. mag. (WC).
• DSRCT - very high mag. (WC).

DDx:

• Metastatic germ cell tumour (DDx of location and age).
• Embryonal RMS.
  • It should be noted that DSRCT, like embryonal RMS, is +ve for desmin!

IHC

Features:

• AE1/AE3 +ve.
• Desmin +ve.
• EMA +ve.

Molecular

• t(11;22)(p13;q12).^[40][41]

Clear cell sarcoma

• Known among pathologists as "soft-tissue melanoma" and "melanoma of the soft parts", as it has a strong morphological resemblance.^[42]
  • Molecular changes and origin distinct from melanoma.
• Incidence: rare soft tissue tumour.

Clinical

• Usually - deep soft tissue or extremities.
• Guarded prognosis.
• First described in 1965.^[43]

Microscopy

Features:^[42]

• Architecture: sheets or fascicular (bundles) arrangement.
• Cells: Spindle cells or epithelioid cells.
• Prominent nucleoli - basophilic.
• Fibrous septae.
• Uniform

Image:

• Clear cell sarcoma (WC).
• Clear cell sarcoma (informaworld.com).

IHC

Features:^[42]

• S100 +ve.
• HMB-45 +ve.
• Melan A (MART-1) +ve; sometimes -ve.
• BCL2 +ve.
• CD57 +ve (usually).

Keratins:

• EMA may be +ve.
• CAM5.2 -ve.
• AE1/AE3 -ve.

Molecular studies

• Chromosomal translocation t(12;22)(q13;q12).^[42]
  • Fusion transcripts:
    • EWSR1-ATF1.
    • EWSR1-CREB1 (GI tract associated).

Synovial sarcoma

General

• Does not arise from cartilage.^[37]
  • Usually close to a joint.
• Young adults or adolescents.

Microscopic

Comes in three (histologic) flavours:^[37][44]

1. Spindle cell sarcoma with features of hemangiopericytoma, i.e. staghorn vessels.
2. Biphasic synovial sarcoma:
   1. Spindle cells with features of hemangiopericytoma.
   2. Epitheliod glands or nests.
3. Primative round cell type.

Images:

• Monophasic synovial sarcoma with staghorn vessels - intermed. mag. (WC).
• Synovial sarcoma (scielo.br).
• Synovial sarcoma - collection of images (humpath.com).

IHC

Features:^[37]

• Vimentin +ve + cytokeratin and/or EMA +ve.
• CD99 +ve.

Others:

• Beta-catenin +ve ~30-70%.^[45]
• Cyclin D1 ~50%.^[45][46]

Molecular pathology

Unique translocation:

• t(X;18)(p11.2;q11.2).^[47]

Other

Granulocytic sarcoma

• AKA myeloid sarcoma, AKA chloroma.

General

• Soft tissue manifestation of acute myeloid leukemia.

Microscopic

Features:

• May mimic small cell carcinoma, small round cell tumours.

See also

• Bone.
• Dermatopathology.
• Hematopathology.
• Spindle cell lesion.
• Neurofibromatosis.
• Small round cell tumours.

References