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Research
2007
:4;
20
doi:
10.1186/1742-6413-4-20

Scope of FNAC in the diagnosis of soft tissue tumors-A study from a tertiary cancer referral center in India

Dept of Pathology, Tata Memorial Centre, Dr E. B. Road, Parel, Mumbai, 400012, India
Clinical Trials Coordinator, Epidemiology & Clinical Trials Unit (ECTU), Advanced Centre for Treatment, Research & Education in cancer (ACTREC), Tata Memorial Centre, Khargar, Navi Mumbai, India
Licence

This is an Open Access article distributed under the terms of the Creative Commons Attribution License, which permits unrestricted use, distribution, and reproduction in any medium, provided the original work is properly cited.

Disclaimer:
This article was originally published by Medknow Publications and was migrated to Scientific Scholar after the change of Publisher.

Abstract

Background

Fine needle aspiration cytology (FNAC) forms one of the first diagnostic tools in the evaluation of tumors. Its role in diagnosing soft tissue tumors (STT) has been fairly documented, as well as debated. Present study was aimed at evaluating its scope in diagnosing 127 cases of soft tissue tumors.

Methods

Conventional Pap and MGG staining was available in all the cases. Immunocytochemistry (ICC) was performed in 15 cases. Histopathological details were available in 115 cases.

Results

50% cases were referred for a primary diagnosis, while 26.8% & 22.8% cases were evaluated for recurrent and metastatic lesions, respectively. Extremities were the commonest sites. On FNAC, 101 cases (79.5%) were labeled as malignant, whereas 10 cases (7.9%) were labeled as benign. The remaining 16 cases (11%) were not categorized and were labeled as ‘unsure/not specified’. Histopathological confirmation in 115 cases, gave a diagnostic accuracy of 98%, with a positive predictive value of 98% in malignant cases and a negative predictive value of 100% in benign cases. Two cases were false positive. Among the various cytological categories, 60 cases (47.2%) were of spindle cell type, followed by 32 (25.2%) of round cell type and 14 cases (11%) of lipomatous type. Other 12 cases (9.4%) were of pleomorphic type; 7 (5.5%) cases of epithelioid type and remaining 2 cases were of myxoid type. All the round cell, pleomorphic and myxoid type of tumors were sarcomas, whereas 73.3% cases of spindle cell type were labeled as ‘malignant’. Exact cytological sub typing was offered in 58 cases, with rhabdomyosarcoma (RMS) as the most frequently sub typed tumor. The two false positive malignant cases were of fibromatosis and a pigmented schwannoma, on biopsy. Out of 28 metastatic lesions, lymph nodes were the commonest site for metastasis, with epithelioid tumors that formed highest percentage of metastatic cases.

Conclusion

FNAC is fairly specific and sensitive in STT diagnoses for primary, recurrent and metastatic lesions. The cytological types, especially round cell and pleomorphic sarcomas, can be quickly identified. Clinicopathological correlation with ICC as an adjunct, are valuable in exact sub typing.

Background

Soft tissue tumors (STT) are rare neoplasms. At our hospital, 2.5% of the cancer cases are constituted by soft tissue sarcomas. Most of these cases are referrals, including a larger proportion of malignant cases, invariably with a high grade and stage. [1] These tumors pose a significant diagnostic challenge as a result of their morphologic overlap and biological heterogeneity [2]. Among its various diagnostic aids, lately, FNAC has been gaining importance as a result of its cheap cost, easy performance, safety, along with fair specificity and specificity, especially in terms of sorting out malignant cases. Apart from its use in recurrent and metastatic cases, FNAC has been identified as a useful diagnostic technique in the initial diagnosis of STTs [38].

The present study was aimed at evaluating 127 cases of FNAC smears from soft tissue tumors, diagnosed over a period of 5 years. The other objectives included identification of cyto-histological concordance in terms of malignancy; stratification of the tumors into various cytomorphological categories and to note the extent of specific sub-typing in individual cases.

Methods

127 aspirates (unaided and guided) from STTs were evaluated over a period of 5 years (2001-2006). Only cases with relevant clinical data were included. All cases included conventional Papanicolaou (Pap) and May Grunwald Giemsa (MGG) stained smears. Inadequate smears were the ones with ‘no’ or scanty cells. Non-neoplastic lesions, on biopsy, were excluded. Histological details, in 115 cases, were accessed from the clinical charts and the Hospital Diagnostic Information System (DIS).

On examination, all cases were placed into 6 cytomorphological categories, namely spindle cell, round cell, pleomorphic, myxoid, epithelioid/polygonal cell and lipomatous type [9]. In cases of mixed components, the specific subtype was assigned based on the predominant morphological pattern. Immunocytochemistry was performed in 15 cases for an exact sub typing, on smears and cell blocks. Exact sub typing was offered in the clinical context, with ICC as an adjunct.

Immunocytochemistry (ICC) technique on smears

Smears were fixed in methanol, followed by 3 changes in 100% absolute alcohol for 5 min each. This was followed by washing under running tap water for 5 min. Next, the smears were subjected to endogenous peroxidase for 30 min (H2O2 + methanol). This was followed by washing under running tap water, antigen retrieval (low heat with microwave or enzyme) and 3 changes of wash with Tris Buffer solution (TBS) ~5 min. Subsequently, blocking serum was applied, followed by incubation with primary antibody ~1 hour and TBS washing. Further, secondary antibody was applied for 30 min, followed by washing with TBS and application of avidin-biotin complex (ABC). Afterwards, TBS washing was carried out with subsequent staining with Diamino Benzidine (DAB) reagent. Harris’ hematoxylin was used as a counter stain. Finally, the smears were dehydrated with absolute alcohol, cleared with xylene and mounted with DPX. The cases were accompanied with appropriate controls. A limited panel of markers was carried out on the smears, including vimentin, desmin, S-100, cytokeratin (CK), MIC-2, myogenin, neuron specific enolase (NSE), synaptophysin, chromogranin and myeloperoxidase (MPO).

Immunohistochemistry (IHC) was performed by immunoperoxidase procedure. On biopsy a wide panel of markers was carried out for exact subtyping. In addition, smooth muscle actin (SMA), Myo D-1, BCL-2, epithelial membrane antigen (EMA), Leukocyte common antigen (LCA), ALK-1, CD30, NSE, synaptophysin and chromogranin (Dako, Produkionsveg, Glostrup, Denmark) constituted as other markers.

Statistical analysis

Statistical analysis was carried out using SPSS (version 14) software. Descriptive analysis was performed using frequency and percentages. In terms of malignancy, cytology was compared with histopathological findings by calculating specificity, sensitivity, and concordance along with positive and negative predictive values (PV). The significance of various cytological categories in terms of benign, malignant and ‘unsure’/not specified’ was analyzed using chi-square test. P value < 0.05 was considered significant.

Results

Out of 127 cases, maximum cases (27, 21.3%) were noted in the age group 21-30 years. Lower extremities were the common sites, with thigh as the most common site of occurrence in 20 cases (15.7%). Males outnumbered the females (1.8:1).

Sixty-four cases (50.4%) were referred for a primary diagnosis, while 34 cases (26.8%) were evaluated for recurrent lesions & remaining 29 cases (22.8%) cases for metastatic disease.

On FNAC, 101 cases (79.5%) were labeled as malignant and 10 cases (7.9%) as benign. 16 cases (14.5%) were labeled as ‘unsure’/‘not categorized’. With biopsy results, finally, 107 cases (84.25%) were labeled malignant/sarcomas; 16 (12.59%) as benign, 2 as borderline/intermediate malignancies and 2 cases were ‘unsure/not specified’. Histopathological confirmation, available in 115 cases (90.5%), gave a diagnostic accuracy of 98% with a positive predictive value of 98% in terms of malignancy and a negative predictive value of 100% in benign cases. The overall sensitivity was 100% and specificity was 83.3%.

Out of the 16 cases that were not categorized, 5 turned out to be benign, 8 malignant and 2 cases as intermediate malignancy, on histopathology. The remaining 2 cases lacked biopsy results.

Among the various cytomorphological categories, 14 cases (11%) were of lipomatous tumors, 12 cases (9.4%) were of pleomorphic type, 32 cases (25.2%) were of round cell type, 60 (47.2%) of spindle cell type, 7 cases (5.5%) of epithelioid type and the remaining 2 cases were of myxoid type. All the round cell, epithelioid, pleomorphic and myxoid tumors were sarcomas. Out of 60 cases of spindle cell subtype, 44 (73.3%) were malignant and 16 cases (26.6%) were not categorized, either as benign or malignant.

The cytological diagnoses included ‘terms’ like spindle cell sarcoma (31 cases), malignant round cell tumor (12 cases), sarcoma of epithelioid type (7 cases), spindle cell tumor (14 cases), and spindle cell lesion (4 cases). Ten benign cases were of lipomas.

Out of 16 ‘unsure’/‘non classified’ cases; on biopsy, 8 cases turned out to be malignant, namely 3 spindle cell sarcomas, 2 MPNSTs, 1 synovial sarcoma, 1 gastrointestinal stromal tumor (GIST) and 1 pleomorphic sarcoma (NOS). The remaining 8 cases included 2 of intermediate malignancy, namely, 1 case, each of a dermatofibrosarcoma protuberans (DFSP) and fibromatosis. Another 1 case was of proliferative fasciits. Another 3 cases included 2 of schwannoma and 1 case of a neurofibroma. Remaining 2 cases could not be categorized due to lack of biopsy results

With the help of clinical details and ICC, exact sub typing was possible in 58 cases. Out of 14 lipomatous tumors, commonest were lipomas (10 cases), including 1 case of a pleomorphic lipoma; 2 cases were of myxoid liposarcomas and remaining 2 cases were of pleomorphic liposarcomas. Out of 60 cases of spindle cell category, specific diagnoses in 14 cases included leiomyosarcoma (3 cases), MPNST (2 cases), synovial sarcoma (3 cases), melanoma of soft parts (1 case). One case was offered a differential diagnosis of MPNST vs. melanoma of soft parts, another of a MPNST vs. synovial sarcoma and remaining 1 case was of sarcoma vs. a sarcomatoid carcinoma (poorly differentiated). In the round cell category, exact sub typing was more possible i.e. in 20 cases that included RMS (10 cases), PNET/Ewing's (9 cases) along with 1 case of a neuroblastoma. In the pleomorphic group, 8 cases were labeled as pleomorphic cell sarcoma, 2 as pleomorphic rhabdomyosarcomas and 1 case as an extraskeletal osteosarcoma. One case was offered a differential of a pleomorphic sarcoma vs. poorly differentiated carcinoma, however, lacked biopsy results.

Out of 7 cases of tumors with epithelioid morphology, all were malignant. The cytological diagnoses included 1 case of an epithelioid sarcoma and 1 case of an epithelioid MPNST. Remaining 5 cases were labeled as sarcomas with an epithelioid morphology. On histopathology, 1 of these turned out as a malignant granular cell tumor; 1 epithelioid leiomyosarcoma; 1 Alk 1 positive anaplastic large cell lymphoma (ALCL) and another 1 as a pleomorphic sarcoma (NOS). One case turned out to be a myxoid liposarcoma with round/polygonal cells, the latter that were seen in the smears. In the myxoid category, both the tumors were designated as myxofibrosarcomas. (Figures 1, 2, 3, 4) While one of these was in the thigh of a 60 years old male, the other case that turned out as a pleomorphic sarcoma, myxoinflammatory type on biopsy, was identified in the leg of a 52 years old male. (Table No. 1, 2, 3, 4)

A. Pleomorphic lipoma. Mature adipose tissue fragments with giant cells (arrow). MGG × 200. B. High power view of ‘Floret-type’ giant cells, displaying ‘wreath-like’ nuclear arrangement. MGG × 400. C. Biopsy of pleomorphic lipoma displaying floret-type giant cells. H&E × 200. D. Myxoid Liposarcoma. Abundant metachromatic, myxoid stroma with vacuolated cells (Lipoblasts) (arrow). MGG × 400. E. Cellular smear showing plexiform capillary network with entrapped lipoblasts (inset) Pap × 200. F. Pleomorphic liposarcoma. Hypercellular smear showing several pleomorphic cells (arrow), including lipoblasts admixed with inflammatory cells. Pap × 400.
Figure 1
A. Pleomorphic lipoma. Mature adipose tissue fragments with giant cells (arrow). MGG × 200. B. High power view of ‘Floret-type’ giant cells, displaying ‘wreath-like’ nuclear arrangement. MGG × 400. C. Biopsy of pleomorphic lipoma displaying floret-type giant cells. H&E × 200. D. Myxoid Liposarcoma. Abundant metachromatic, myxoid stroma with vacuolated cells (Lipoblasts) (arrow). MGG × 400. E. Cellular smear showing plexiform capillary network with entrapped lipoblasts (inset) Pap × 200. F. Pleomorphic liposarcoma. Hypercellular smear showing several pleomorphic cells (arrow), including lipoblasts admixed with inflammatory cells. Pap × 400.
A. Rhabdomyosarcoma (RMS). Hypercellular smear with round cells, including plasmacytoid and binucleate forms (arrow), against a ‘lacy’ background MGG × 200. B. Smear with singly scattered round cells and an isolated strap cell/tumor rhabdomyoblast (arrow). Pap × 200. C. Diffuse desmin positivity in the round cells. DAB × 400. D. Alveolar RMS. Hypercellular smear with round cells including ‘wreath’-like giant cells (inset). Pap × 400. E. High power view of an isolated wreath-like giant cell. Pap × 400. F. Cell block preparation showing strong myogenin expression. DAB × 400. G. PNET. Hypercellular smear with round cells, scattered singly and forming ‘rosettes’ (arrow). H. Positive MIC2 (CD99) expression in the tumor cells (DAB × 400). I. Neuroblastoma. Smear displaying round cells, with fine nuclear chromatin and exhibiting Homer-wright rosettes. J. High power view of an isolated pseudo rosette. L. Granulocytic sarcoma (formed on biopsy). Malignant round cell tumor, showing blasts. Strong MP0 positivity, on imprint, in the tumor cells. (DAB × 200).
Figure 2
A. Rhabdomyosarcoma (RMS). Hypercellular smear with round cells, including plasmacytoid and binucleate forms (arrow), against a ‘lacy’ background MGG × 200. B. Smear with singly scattered round cells and an isolated strap cell/tumor rhabdomyoblast (arrow). Pap × 200. C. Diffuse desmin positivity in the round cells. DAB × 400. D. Alveolar RMS. Hypercellular smear with round cells including ‘wreath’-like giant cells (inset). Pap × 400. E. High power view of an isolated wreath-like giant cell. Pap × 400. F. Cell block preparation showing strong myogenin expression. DAB × 400. G. PNET. Hypercellular smear with round cells, scattered singly and forming ‘rosettes’ (arrow). H. Positive MIC2 (CD99) expression in the tumor cells (DAB × 400). I. Neuroblastoma. Smear displaying round cells, with fine nuclear chromatin and exhibiting Homer-wright rosettes. J. High power view of an isolated pseudo rosette. L. Granulocytic sarcoma (formed on biopsy). Malignant round cell tumor, showing blasts. Strong MP0 positivity, on imprint, in the tumor cells. (DAB × 200).
A. Malignant peripheral nerve sheath tumor. Hypercellular smear showing loosely cohesive spindly cells with indented, ‘serpentine’ nuclei Pap × 400. B. Tumor cells showing S-100 positivity on cellblock preparation. DAB × 400. C. Leiomyosarcoma. Hypercellular smear showing fragments and singly scattered cells with blunt-ended nuclei. Pap × 400. D. Endometrial stromal sarcoma (ascertained on biopsy). Hypercellular smear with ovoid cells and abundant metachromatic basement membrane material. MGG × 200. F. Synovial sarcoma. Hypercellular smear with oval to elongated cells exhibiting overlapping. Pap × 200. G. A recurrent synovial sarcoma showing biphasic cellular pattern and eosinophilic material on smears. MGG × 400. H. Melanoma of soft parts. Cellular smear with spindly cells displaying prominent nucleolisation (inset). Pap × 400. I. Strong S-100 positivity on smears. DAB × 400 (Inset, S-100 highlighting spindly processes. DAB × 1000). J. Myxofibrosarcoma. Moderately cellular smear with oval cells admixed with metachromatic myxoid stroma. MGG × 200. K. Curvilinear vascular pattern with cells around. MGG × 400. L. Pleomorphic Rhabdomyosarcoma. Hypercellular smear with markedly pleomorphic cells. Pap × 400. Inset showing a pleomorphic rhabdomyoblastic cell. Pap × 400. M. Pleomorphic sarcoma not otherwise specified (NOS). Hypercellular smear with markedly pleomorphic cells against a hemorrhagic background. MGG × 400.
Figure 3
A. Malignant peripheral nerve sheath tumor. Hypercellular smear showing loosely cohesive spindly cells with indented, ‘serpentine’ nuclei Pap × 400. B. Tumor cells showing S-100 positivity on cellblock preparation. DAB × 400. C. Leiomyosarcoma. Hypercellular smear showing fragments and singly scattered cells with blunt-ended nuclei. Pap × 400. D. Endometrial stromal sarcoma (ascertained on biopsy). Hypercellular smear with ovoid cells and abundant metachromatic basement membrane material. MGG × 200. F. Synovial sarcoma. Hypercellular smear with oval to elongated cells exhibiting overlapping. Pap × 200. G. A recurrent synovial sarcoma showing biphasic cellular pattern and eosinophilic material on smears. MGG × 400. H. Melanoma of soft parts. Cellular smear with spindly cells displaying prominent nucleolisation (inset). Pap × 400. I. Strong S-100 positivity on smears. DAB × 400 (Inset, S-100 highlighting spindly processes. DAB × 1000). J. Myxofibrosarcoma. Moderately cellular smear with oval cells admixed with metachromatic myxoid stroma. MGG × 200. K. Curvilinear vascular pattern with cells around. MGG × 400. L. Pleomorphic Rhabdomyosarcoma. Hypercellular smear with markedly pleomorphic cells. Pap × 400. Inset showing a pleomorphic rhabdomyoblastic cell. Pap × 400. M. Pleomorphic sarcoma not otherwise specified (NOS). Hypercellular smear with markedly pleomorphic cells against a hemorrhagic background. MGG × 400.
Tumors with epithelioid/polygonal shapes, exactly categorized on biopsy. A. Epithelioid sarcoma (recurrent case). Hypercellular smear with polygonal cells, scattered singly, displaying fine vacuoles in a minority of cells (inset). Pap × 400. B. Anaplastic large cell lymphoma. Hypercellular smear with singly scattered cells revealing moderate to abundant, eosinophilic to finely vacuolated cytoplasm and pleomorphic nuclei. MGG × 400. C. Malignant granular cell tumor. Hypercellular smear with loosely cohesive and singly scattered cells exhibiting ovoid nuclei and abundant, granular, eosinophilic cytoplasm. Pap × 200. C. Diffuse S-100 positivity in tumor cells on IHC on biopsy. DAB × 200.
Figure 4
Tumors with epithelioid/polygonal shapes, exactly categorized on biopsy. A. Epithelioid sarcoma (recurrent case). Hypercellular smear with polygonal cells, scattered singly, displaying fine vacuoles in a minority of cells (inset). Pap × 400. B. Anaplastic large cell lymphoma. Hypercellular smear with singly scattered cells revealing moderate to abundant, eosinophilic to finely vacuolated cytoplasm and pleomorphic nuclei. MGG × 400. C. Malignant granular cell tumor. Hypercellular smear with loosely cohesive and singly scattered cells exhibiting ovoid nuclei and abundant, granular, eosinophilic cytoplasm. Pap × 200. C. Diffuse S-100 positivity in tumor cells on IHC on biopsy. DAB × 200.
Table 1 Various cases of spindle cell tumors with FNAC and histopathologic diagnoses
Sr No. Age Gender Site FNAC Diagnosis Histopathology Diagnosis Concordance
1 43 M Thigh Spindle cell sarcoma Synovial sarcoma 1
2 30 M Thigh Spindle cell sarcoma Synovial sarcoma 1
3 62 F Retroperitoneum Spindle cell sarcoma NK 3
4 55 F Chest wall Spindle cell sarcoma NK 3
5 65 M Retroperitoneum Spindle cell sarcoma NK 3
6 64 M Axilla Spindle cell sarcoma NK 3
7 56 M Leg Spindle cell sarcoma Spindle cell sarcoma 1
8 57 M Retroperitoneum Spindle cell sarcoma Spindle cell sarcoma 1
9 21 M Skull Spindle cell sarcoma MPNST 1
10 34 F Iliac Fossa Spindle cell sarcoma NK 3
11 29 M Heel Synovial sarcoma Synovial sarcoma 1
12 27 F Uterus Leiomyosarcoma endometrial stromal sarcoma 1
13 56 M Abdominal wall Spindle cell tumor Spindle cell sarcoma 2
14 26 M Arm Spindle cell tumor MPNST 2
15 54 M Iliac Fossa Spindle cell tumor GIST 2
16 48 M Neck Leiomyosarcoma Leiomyosarcoma 1
17 37 M Pleura Spindle cell tumor Schwannoma 2
18 50 M Posterior Mediastinum MPNST MPNST 1
19 62 M Forearm Spindle cell tumor-Neurogenic MPNST 2
20 48 F Uterus Spindle cell sarcoma Leiomyosarcoma 1
21 40 F Intra abdominal Spindle cell tumor NK 3
22 50 F Uterus Sarcoma vs poorly differentiated carcinoma Leiomyosarcoma 1
232 50 F Uterus Leiomyosarcoma Leiomyosarcoma 1
4 34 M Paraspinal Melanoma vs MPNST Pigmented schwannoma 4
25 51 M Intra abdominal Spindle cell tumor DFSP 2
26 25 F Lumbar MPNST MPNST 1
27 25 M Iliac Fossa Spindle cell sarcoma NK 3
28 51 M Arm Spindle cell tumor Proliferative Fascitis 2
29 40 M Heel Clear cell sarcoma/Melanoma Clear cell sarcoma/Melanoma 1
30 52 F Leg Synovial sarcoma Synovial sarcoma 1
31 66 M Suprascapular Spindle cell sarcoma Spindle cell sarcoma 1
32 51 M Arm Spindle cell sarcoma Leiomyosarcoma 1
33 66 M Neck Spindle cell tumor NK 3
34 29 F Ovary Spindle cell sarcoma Spindle cell sarcoma 1
35 22 F Intra abdominal Spindle cell lesion Fibromatosis 2
36 22 M Maxilla Spindle cell sarcoma MPNST 1
37 68 M Foot Spindle cell sarcoma Spindle cell sarcoma 1
38 35 M Maxilla Spindle cell lesion Spindle cell sarcoma 2
Sr No. Age Gender Site FNAC Diagnosis Histopathology Diagnosis Concordance
39 35 F Thigh Spindle cell sarcoma Fibrosarcoma 1
40 39 F Thigh Spindle cell sarcoma Spindle cell sarcoma 1
41 35 F Thigh Spindle cell sarcoma Fibromatosis 4
42 28 F Scapula Spindle cell sarcoma: Synovial/vs MPNST Synovial sarcoma 1
43 47 M Occiput Spindle cell tumor Pleomorphic sarcoma 2
44 28 M Thorax Spindle cell lesion Neurofibroma 2
45 20 F Thigh Spindle cell sarcoma MPNST 1
46 40 M Thigh Spindle cell sarcoma Spindle cell sarcoma 1
47 32 F Neck Spindle cell sarcoma Spindle cell sarcoma 1
48 25 F Arm Spindle cell sarcoma Synovial sarcoma 1
49 55 F Lung Spindle cell tumor Spindle cell tumor 1
50 13 M Leg Spindle cell sarcoma MPNST 1
51 30 M knee Synovial sarcoma Synovial sarcoma 1
52 32 M Neck Spindle cell sarcoma Synovial sarcoma 1
53 30 F Neck Spindle cell lesion Spindle cell sarcoma 2
54 24 F Poplitial Fossa Spindle cell tumor Synovial sarcoma 2
55 40 F Thigh Spindle cell sarcoma NK 3
56 56 M Leg Clear cell sarcoma/melanoma Clear cell sarcoma/melanoma 1
57 23 M Foot Spindle cell sarcoma Synovial sarcoma 1
58 67 M Neck Spindle cell sarcoma Spindle cell sarcoma 1
59 47 F Arm Spindle cell tumor Schwannoma 2
60 22 M Popliteal Fossa Spindle cell sarcoma MPNST 1

Key: Concordance: 1: Concordant; 2: Not specified; 3: Couldn’t be ascertained; 4: Discordant M: Male, F: Female

Table 2 Various cases of round cell tumors with FNAC and histopathologic diagnoses
Sr No. Age Gender Site FNAC Diagnosis Histopathology Diagnosis Concordance
1 2 M Orbit Rhabdomyosarcoma Rhabdomyosarcoma 1
2 14 M Hand Rhabdomyosarcoma Rhabdomyosarcoma 1
3 11 M Chest wall Round cell sarcoma Rhabdomyosarcoma 1
4 18 F Orbit Rhabdomyosarcoma Rhabdomyosarcoma 1
5 2 M Thigh PNET/Ewing's sarcoma PNET/Ewing's sarcoma 1
6 27 M Thigh PNET/Ewing's sarcoma PNET/Ewing's sarcoma 1
7 25 M Iliac Fossa PNET/Ewing's sarcoma PNET/Ewing's sarcoma 1
8 25 M Iliac Fossa PNET/Ewing's sarcoma PNET/Ewing's sarcoma 1
9 30 F Neck Sarcoma – Epithelioid PNET/Ewing's sarcoma 1
10 19 M Thigh Malignant round cell tumor PNET/Ewing's sarcoma 1
11 46 F Neck Malignant round cell tumor PNET/Ewing's sarcoma 1
12 5 F Thigh Rhabdomyosarcoma Rhabdomyosarcoma 1
13 16 M Maxilla Rhabdomyosarcoma Rhabdomyosarcoma 1
14 17 F Thigh Rhabdomyosarcoma Rhabdomyosarcoma 1
15 18 M Scalp Rhabdomyosarcoma Rhabdomyosarcoma 1
16 3 M Leg Rhabdomyosarcoma Rhabdomyosarcoma 1
17 19 M Neck Rhabdomyosarcoma Rhabdomyosarcoma 1
18 1 M Paraspinal Round cell sarcoma Rhabdomyosarcoma 1
19 30 F Gluteal PNET/Ewing's sarcoma PNET/Ewing's sarcoma 1
20 5 F Scapula Malignant round cell tumor Neuroblastoma 1
21 8 M Leg Malignant round cell tumor Rhabdomyosarcoma 1
22 9 M Intra abdominal Malignant round cell tumor Rhabdomyosarcoma 1
23 2 M Orbit Malignant round cell tumor Retinoblastoma 1
24 3 M Gluteal Round cell sarcoma NK 3
25 4 F Chest wall PNET/Ewing's sarcoma PNET/Ewing's sarcoma 1
26 1 F Orbit Neuroblastoma Neuroblastoma 1
27 22 M Scalp Malignant round cell tumor Granulocytic sarcoma 1
28 13 M Chest wall PNET/Ewing's sarcoma PNET/Ewing's sarcoma 1
29 20 F Axilla PNET/Ewing's sarcoma PNET/Ewing's sarcoma 1
30 35 M Iliac Fossa PNET/Ewing's sarcoma PNET/Ewing's sarcoma 1
31 16 M Iliac Fossa Malignant round cell tumor DSRCT 1
32 6 F Maxilla Rhabdomyosarcoma (alveolar) Rhabdomyosarcoma (alveolar) 1

Key: Concordance: 1: Concordant; 2: Not specified; 3: Couldn’t be ascertained; 4: Discordant M: Male, F: Female

Table 3 Various cases of epithelioid tumors with FNAC and histopathologic diagnoses
Sr No. Age Gender Site FNAC Diagnosis Histopathology Diagnosis Concordance
1 68 M Back Epithelioid sarcoma Epithelioid sarcoma 3
2 47 M Thigh Epithelioid MPNST Epithelioid MPNST 1
3 28 M Leg Sarcoma – Epithelioid Leiomyosarcoma 1
4 58 F Thigh Sarcoma – Epithelioid Myxoid liposarcoma 1
5 65 M Shoulder Sarcoma – Epithelioid Pleomorphic sarcoma (NOS) 1
6 43 M Thigh Sarcoma – Epithelioid Malignant Granular cell tumor 1
7 16 M Elbow Sarcoma – Epithelioid Anaplastic Large cell Lymphoma 1

Key: Concordance: 1: Concordant; 2: Not specified; 3: Couldn’t be ascertained; 4: Discordant M: Male, F: Female

Table 4 Various cases of pleomorphic tumors with FNAC and histopathologic diagnoses
Sr No. Age Gender Site FNAC Diagnosis Histopathology Diagnosis Concordance
1 49 M Scapula Pleomorphic cell sarcoma Pleomorphic sarcoma (NOS) 1
2 45 M Chest wall Pleomorphic sarcoma, myogenic Pleomorphic sarcoma rhabdomyosarcoma 1
3 19 M Leg Pleomorphic cell sarcoma Pleomorphic sarcoma (NOS) 1
4 50 F Chest wall Pleomorphic Sarcoma vs poorly differentiated carcinoma NK 3
5 37 F Thigh Pleomorphic cell sarcoma Osteosarcoma 1
6 9 F Arm Pleomorphic cell sarcoma Osteosarcoma 1
7 19 M Leg Pleomorphic cell sarcoma; Osteosarcoma Osteosarcoma 1
8 33 M Forearm Pleomorphic rhabdomyosarcoma Pleomorphic rhabdomyosarcoma 1
9 39 M Temporal region Pleomorphic cell sarcoma Pleomorphic liposarcoma 1
10 55 M Retroperitoneum Pleomorphic cell sarcoma NK 3
11 60 F Inguinal Pleomorphic cell sarcoma Pleomorphic sarcoma (NOS) 1
12 50 M Chest wall Pleomorphic cell sarcoma Pleomorphic sarcoma (NOS) 1

Key: Concordance: 1: Concordant; 2: Not specified; 3: Couldn’t be ascertained; 4: Discordant M: Male, F: Female

Twenty-eight cases (22%) presented with metastatic deposits, commonly in lymph nodes (16 cases, 57.1%), followed by liver and lungs as the next commonest sites. Highest numbers of cases revealing metastatic deposits were of spindle cell type. However, the highest percentage of cases was of epithelioid category (28.5%), followed by pleomorphic (25.5%), spindle cell (25%), round cell category (18.75%) and finally; lipomatous tumors (14.2%). In terms of exact subtypes, RMS (6 cases) was the commonest tumor to metastasize, followed by leiomyosarcoma (5 cases), synovial sarcoma (4 cases) and pleomorphic sarcoma (4 cases).

Discussion

Soft tissue tumors (STTs) have been diagnosed with the ‘time-honored’ histopathology that is recognized as the ‘gold standard’ for their evaluation. However, in the current era, where ‘needle is preceding the scalpel’ and the biopsy material is getting limited, it would be prudent to discuss the role and scope of FNAC in diagnosing STTs. The role of FNAC has mostly been noted in soughting recurrent and metastatic STT cases [68]. Nevertheless, there are studies indicating its role in primary diagnosis of these tumors [35]. The present study was carried out to highlight various aspects of cytological diagnosis of STTs, in a series of 127 cases, wherein maximum cases (50%) were submitted exclusively for a primary diagnosis. An increased number of overall malignant (84.25%) vs. benign cases (12.5%) in our series were comparable to a study by Miralles et al [10] and contrasting to another other study [11]. The reason was the predominance of referral cases, including a greater proportion of sarcomas that our center receives. Moreover, non-neoplastic lesions were excluded in this study.

In terms of diagnosis, complex heterogeneity of STTs is known to be a limiting factor in their exact categorization. With the advent of ancillary techniques like IHC, flow cytometry, cytogenetics and molecular techniques, the objectivity of diagnosing a STT has been considerably enhanced. In a study, Kilpatrick et al [4] have presented the extent to which cytology can be utilized in effective diagnosis of STTs. Subsequently, there have been studies highlighting application of the ancillary techniques in exact sub typing of these tumors [781213]. Apart from providing material for these studies, FNAC is easy, safe and cost effective. While the fear of tumor seedling is hardly noted, its effectivity is best exemplified with more access to mass lesions in form of multiple aspirates [4]. In our series, none of the cases had complications or tumor seedlings.

In terms of diagnostic efficacy, 100% sensitivity and 87% specificity in our cases was comparable to results of Nagira et al [11], wherein the respective values were 92% and 97% respectively. In another series, Wakely et al [14] reported 100% sensitivity and 97% specificity in STT diagnosis with FNAC. Layfield et al [3] achieved 95% sensitivity and specificity while dealing with these lesions. In our study, 2 cases (1.57%) were false positive (FP) and none was false negative (FN). While a study on 517 STT aspirates by Akerman et al [15] revealed a 2.9% false positive rate, the subsequent studies by Wakely et al [14] and by Kilpatrick et al [4] yielded a single case of false negativity and nil false positivity. This was in contrast to a study by Nagira et al [11], who identified higher figures for false positivity and false negativity. Our results were comparable to the documented range of < 1%-5% (FP) and 2-15% (FN) [341116]. Nil FN in our series was due to the fact that 16 cases were diagnosed as ‘unsure’/not specified. Out of these 8 turned out to be malignant, 1 of intermediate malignancy and 5 benign, on biopsy. An overall concordance of 98% is comparable to results of Shah et al [17].

A basic cytological approach towards making a STT diagnosis begins with the familiarity with normal structures, along with myxoid or metachromatic stromal fragments and a variety of dyscohesive cells like spindly, round, pleomorphic, polygonal that are indicators of a STT, on aspirates [918]. These features are integrated with clinico radiological findings. The value of radiological findings has been fairly discussed [1119]. Infact, improved localization of the ST lesion with radiological techniques has revolutionized the amount of aspirate one can achieve, especially in deep-seated lesions. An adequate aspirate is analyzed and non-neoplastic lesions are sorted out. This is followed by placing neoplastic lesions in benign, borderline/intermediate and malignant groups. This approach was followed in the present study, with the exclusion of secondary soft tissue deposits of carcinomas. The sarcomas were not graded similar to a study by Nagira et al [11], even though attempts at cytologic grading of sarcomas have been made [20]. In their study, Mathur et al [20] identified a low concordance of cytological grading in cases of grade 1 vs. high-grade sarcomas. Our series focused upon the value of cytomorphological sub typing into the six categories, as noted earlier [911]. While all 32 cases of round cell category; 7 of epithelioid type; 12 of pleomorphic type and 2 of myxoid type were placed into malignant groups, 44 of the total 60 cases (73.3%) of spindle cell type could be labeled as sarcomas. Of the remaining 16 cases, 8 turned out to be malignant; 2 of borderline malignancy and 4 as benign. Remaining 2 cases could not be ascertained, in view of lack of biopsy results. The relationship between cytological categorization with benignancy or malignancy of the subtypes was statistically significant. Among the lipomatous group, more cases (10/14) were benign than malignant (4/14). (p < 0.05). While the results for round cell, pleomorphic and lipomatous tumors were comparable to the findings of Nagira et al [11]; we observed more cases of spindle and all of polygonal and myxoid types, as malignant. The reasons include referral of mostly malignant cases to our centre.

In terms of exact sub typing, which was offered in 58 cases, all lipomatous and 70% pleomorphic tumors were suitably categorized. One case of a pleomorphic lipoma showed presence of mature fibroadipose fragments with ‘floret-like’ giant cells, displaying nuclear molding. Presence of this tumor in a superficial location i.e. neck, in an elderly male, was a helpful clue in ruling out a liposarcoma [21]. 70% of pleomorphic sarcomas were categorized in congruence with histopathology. Four out of 10 cases could not be categorized, even on histology with IHC. The reason is the referral of poorly differentiated sarcomas to our center. In their study, Berardo et al [22] concluded lack of any cytological features that could differentiate between malignant fibrous histiocytomas with other pleomorphic sarcomas.

Further, 21 cases of round cell tumors, 13 of spindle cell tumors; 2 cases of myxoid type and 2 cases of epithelioid type were ascertained an exact subtype. Maximum cases in the round cell group were of rhabdomyosarcoma and PNET/Ewing’s. These diagnoses were confirmed with desmin positivity in the former and CD99 positivity in few of the latter cases. One case of an RMS, with an alveolar component, was formed in view of presence of several ‘wreath-like’ giant cells. This was confirmed with positive desmin and myogenin staining on ICC, along with positive Myo-D1 expression, on IHC. Further, positive PAX3-FKHR analysis confirmed the alveolar component [23]. One case of soft tissue neuroblastomas showed neuropils and false rosettes. This was objectively confirmed with NSE positivity and MIC2 negativity. Neuroblastomas were lesser in number in our study, as these tumors are well diagnosed with imaging findings, biochemical tests and biopsy, at our Center. FNAC was carried out in few cases.

Among spindle cell tumors, specific diagnoses were assigned in few cases viz. leiomyosarcoma, MPNST, synovial sarcoma in 3 cases and melanoma in 1 case. While the former 2 were substantiated with clinical details, including location, synovial sarcoma was diagnosed based on specific cytomorphological features. Diagnosis of synovial sarcoma in 3 cases included 2 metastatic cases and one recurrent case. Cytomorphology of synovial sarcoma on cytology is complex. In unusual situations, ICC and t (x: 18) translocations (SYT-SSX) can be useful in forming this exact subtype [1324]. One case of melanoma of soft parts was ascertained with prominently nucleolated spindly cells and few polygonal cells that exhibited diffuse S-100 positivity. This was confirmed with additional HMB45 positivity, on IHC [25]. On biopsy, level of exact subyping was significantly increased in spindle cell tumors. Another case of an endometrial stromal sarcoma was presumed to be a leiomyosarcoma, on FNAC. Retrospectively, presence of hypercellular smears with ovoid cells and prominent basement membrane-like material reminiscent of proliferating vessels were identified as useful features. Recently, a similar case has been reported [26]. Out of 16 cases that were not classified, 4 turned out benign on biopsy. The remaining 8 cases included 2 of intermediate malignancy, namely, 1 case, each of a dermatofibrosarcoma protuberans (DFSP) and fibromatosis. Another 1 case was of proliferative fasciits, on biopsy. In case of adequate material and typical clinical settings, diagnosis of a DFSP can be suggested [27]. The other daunting tumor is fibromatosis that is recognized as a pitfall in STT diagnosis [3513]. This was identified as 1 false positive case in our study, along with another case of MPNST that turned out to be a pigmented schwannoma, on histopathology.

While 2 myxoid tumors were termed as myxofibrosarcomas, one of these turned out to be a pleomorphic sarcoma, myxoinflammatory type. Lack of exact categorization of sarcomas with epithelioid morphology (5 cases) was due to limited cellularity and tumor heterogeneity. One case labeled as sarcoma with epithelioid morphology turned out to be a myxoid liposarcoma, with a round/polygonal cell component. The remaining 2 cases in this category were unusual. While one case turned out to be a malignant granular cell tumor, the other was an Alk-1 positive ALCL. Granular cell tumors have been recognized as a pitfall in FNAC of breast lesions [28]. The diagnosis was ascertained with S100 positivity, on biopsy [29]. The case of an Alk1 + ALCL was noted in a young adolescent male, with multifocal lesions Smears showed dyscohesive polygonal cells with multilobated nuclei and moderate amount of finely vacuolated cytoplasm [30]. Positivity for LCA, CD30, EMA and Alk-1 confirmed this diagnosis, on biopsy. The morphological overlapping was observed between epithelioid and round cell type; between spindle cell and polygonal type in case of melanoma of soft parts, as well as between pleomorphic and lipomatous group in 2 pleomorphic liposarcomas. Nonetheless, cytomorphological categorization helped in building up an algorithmic approach towards exact sub typing.

While Costa et al [31] achieved 20.9% rates in terms of exact sub typing of sarcomas, we, like Nagira et al [11], observed an overall higher rate. In their review, Kilpatrick et al [4] have presented a range of 21–74% of exact sub typing of sarcomas, based on various studies. Exact sub typing can be increased with application of ICC [13]. In the present study, routine ICC was attempted in limited cases; mostly of the round cell type, as exact sub typing in these cases has a definite bearing on management. Maximum cases that lacked exact sub typing were of the spindle cell type. Thirteen cases were diagnosed as spindle cell sarcomas, even on histology. The reasons in many of these included referral cases with lack of paraffin blocks and negativity of a specific lineage, even with IHC, in the remaining few. Exact sub typing of spindle cell tumors is a limiting factor, even in other studies [9]. Prognostication of soft tissue sarcomas has been recommended with histological grading and staging [32]. Recent studies [3334] on cytomorphology of leiomyosarcomas and neurogenic tumors constitute an ‘add-on’ to refining the existing cytomorphology of these subtypes.

Apart from its primary diagnosis; the role of FNAC is recognized in metastatic STT evaluation [78]. Evaluation of ‘foreign cells’ in metastatic locations, in cases with known clinical context, is less challenging than in situations initial metastatic presentations. In such cases, clinical details are imperative before ascertaining a diagnosis. In our series, out of 28 cases with metastatic lesions, maximum metastatic deposits were reported in lymph nodes (55.1%), ‘more-so’ of the groin, followed by liver and lungs. While lymph nodes have been observed as the commonest metastatic location in earlier studies [78], in our study, groin nodes, were found to be more commonly involved. This might be as a result of more STS occurring in extremities. While maximum metastatic cases were of spindle cell type (considering their higher absolute number), the percentage was highest with epithelioid tumors. This is because of tendency of sarcomas, with epithelioid morphology, to have increased chances for metastasis, like carcinomas. An earlier series observed RMS as the commonest metastasizing tumor [8]. In terms of exact subtypes, RMS was the commonly metastasizing tumor in our series.

To sum up, FNAC has a definite role in the diagnosis of STTs in primary, recurrent and metastatic lesions, for a timely management. Cytological categorization is effective, especially for sorting out round cell and pleomorphic tumors. Spindle and epithelioid cell tumors are challenging, especially in terms of exact sub typing. Exact sub tying can be enhanced with applications of ICC. Recognition of ‘pitfall’ lesions like aggressive fibromatosis is vital. Further scope of STT evaluation on cytology can be increased with more studies dealing with application of ancillary techniques on aspirate samples.

Competing interests

The author(s) declare that they have no competing interests.

Authors' contributions

ACK: Description of data and statistical analysis.

BDG: Retrieval of cases, involved in review of cases.

BR: Study design, review of cases, data analysis and preparation of the manuscript

RFC: Overall supervision and has given the final approval of the manuscript.

The study was presented as a poster at the 16th International Congress of Cytology from 13th–17th May 2007 at Vancouver, BC, Canada.

We would like to thank Mr Mahendra Palker and Mrs Rekha Thorat from the IHC lab for carrying out immunocytochemistry (ICC) and IHC.

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