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International Clinical Pathology Journal

Research Article Volume 4 Issue 6

Histomorphological study of soft tissue tumors and review of literature of rarer types

Gayatri Gogoi,1 Mondita Borgohain,2 Projnan Saikia,3 Brinkal Patel,4 RK Hazarika,5 RC Brahma,6 Bidit Gogoi,7 Nabajyoti Saikia,8 Jolly Rabha9

1Assistant Professor of Pathology, Assam Medical College, India
1Assistant Professor of Pathology, Assam Medical College, India
2Professor of Pathology, Assam Medical College, India
2Professor of Pathology, Assam Medical College, India
3Professor of Pathology, Assam Medical College, India
3Professor of Pathology, Assam Medical College, India
4Graduate Trainee of Pathology, Assam Medical College, India
4Graduate Trainee of Pathology, Assam Medical College, India
5Professor of Pathology, Assam Medical College, India
5Professor of Pathology, Assam Medical College, India
6Associate Professor of Surgery, Assam Medical College, India
6Associate Professor of Surgery, Assam Medical College, India
7Demonstrator of Pathology, Assam Medical College, India
7Demonstrator of Pathology, Assam Medical College, India
8Associate Professor of Otolaryngology, Assam Medical College, India
8Associate Professor of Otolaryngology, Assam Medical College, India
9Assistant Professor, Pediatrics, Assam Medical College, India
9Assistant Professor, Pediatrics, Assam Medical College, India

Correspondence: Gayatri Gogoi, Assistant Professor of Pathology, Assam Medical College, Dibrugarh, Assam, India, Tel -9435029993

Received: January 01, 1971 | Published: June 16, 2017

Citation: Gogoi G, Borgohain M, Saikia P, et al. Histomorphological study of soft tissue tumors and review of literature of rarer types. Int Clin Pathol J. 2017;4(6):151–161. DOI: 10.15406/icpjl.2017.04.00113

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Abstract

Soft tissue tumors constitute a large and heterogeneous group of neoplasms. Clinically soft tissue tumors range from benign, self limited lesions to intermediate grade to highly Aggressive. Most of soft tissue tumors are benign, while few of them are malignant in nature. It ranges from most common benign tumours to some of the rare malignant soft tissue tumors. Our aim was to study the histomorphological patterns and features with review of literature of few rare malignant soft tissue tumours the retrospective study was carried in department of pathology, from January 1, 2013 to December 31, 2014. A record was taken from total 5895Patients; among them total 794cases of soft tissue tumors were noted. Out of which 733cases were found to be benign (92.8%) and 61cases turned out to be malignant (7.2%). The most common benign tumor was leiomyoma (52%) followed by Haemangioma (16%) and Lipoma (10.1%) and common malignant tumor was Fibrosarcoma followed br Rhabdomyosarcoma. Among 794cases, 183 tumors were diagnosed in male, while 611 cases were diagnosed in females. The most common site involved was extremities.

Keywords: soft tissue, tumors, benign, malignant, leiomyoma, hemangioma, lipoma, fibrosarcoma, immunohistochemistry

Introduction

Soft tissue refers to non-epithelial tissue; it is supporting tissue which are extra skeletal excluding joints, central nervous system, skeleton, haematopoietic and lymphoid tissues. Soft tissue tumors can occur at any age. It has been noted that the histological distribution of soft tissue tumors are rather specific for a particular age group at a particular anatomical site.1,2 Both benign and malignant soft tissue tumors commonly present as a painless mass. Examples of soft tissues are Adipose tissue, Fibrous tissue, Vascular tissue, skeletal muscle tissue, Smooth muscle and Nerve sheaths. Tumors range from benign, self limited lesions to highly aggressive malignant with significant risk of metastasis and high mortality.

Soft tissue tumors have wide morphological as well as histological variation that can be detected by microscopic examination. Soft tissue tumors are uncommon and comprise about 2% or less of the cases. As benign soft tissue tumors outnumber their malignant counterpart, this tumors more or less resembles the normal tissues. There are special techniques that have been successfully applied to increase diagnostic accuracy; these include conventional special stains, electron microscopy, immunohistochemistry and cytogenetic/molecular methods. They arise nearly everywhere in the body, the most important locations being the extremities, trunk, abdominal cavity and head & neck region.3

There is no known predisposing cause but majority of them arises sporadic. Unlike tumors like carcinoma that usually arises from recognized precursor lesions; the origin of sarcomas is unknown. It has been postulated that the tumors arises from pluripotent mesenchymal stem cells, which acquires somatic driver mutation in ongogenes and tumor suppressor genes. Reports have linked specific genetic, immunodeficiency, viral infection and environmental factors with the development of some STS. Environmental factors (e.g., radiation, herbicides) have been associated with the development of specific types of sarcomas.4–8 Some sarcomas have a higher predisposition to occur in the setting of familial cancer syndromes (e.g., retinoblastoma syndrome, Li-Fraumeni syndrome, hereditary leiomyomatosis and renal cell carcinoma).9–12 These observations suggest that both environmental and genetic factors are important in the development of these tumors.

Aims and objectives

  1. To study histomorphology and characteristic patterns of different soft tissue tumours.
  2. 2. To describe the difficulties and application of immunohistology in confirmation.
  3. Review of literature of few rare malignant tumours.

Material and methods

It was a descriptive study of Soft tissues tumors over a period of 2 years (January 2013- to December 2014) conducted in the Department of Pathology, in Histopathology and immunohistochemistry Laboratory of Assam Medical Hospital and College, Dibrugarh. Total records of 5895 patients were verified in documentation section. Relevant formalin fixed paraffin embedded blocks in archive of Pathology were retrieved .The Standard operating procedure to receive samples in histopathological laboratory from different departments and operation theatures was with proper identification, labeling and origin. The format contains basic informations such as Name, Age, Sex, Hospital No, Specimen No, Date of specimen collected, Location of tumor and Clinical presentation and other investigations findings. The Histopathology tissue processing protocol involved fixation in 10% buffered formalin (PH 7.2-7.4) with volume 10 times more of tissue size for 12-36 hours according to type of specimen. Additionally bony tissues were decalcified to remove calcium salt. The grossing were carried out on same day or next day with special emphasis to location, size in 3 dimensions of specimen, Morphological features of tissue and tumor, size of tumor and other representative areas. At least 4 Sections from tumour and one from each margins in general were taken in appropriate size to fit the cassettes and were labeled, which were kept in 10% formalin as mentioned The sections were processed under standardized condition for dehydration using acetone for 2 hours, changing acetone every 30 minutes followed by process of clearing using Benzene for 30 minutes and later paraffin embedding and block making.

Diagnosis of soft tissue tumour blocks .The slides were reviewed to record histopathological details in the study Performa. An additional slide of a thickness of tissue 4-5 microns were made with help of Rotary microtome and prepared for routine stain with Haematoxylin and Eosin to examine under light microscope for histopathological features followed by ascertaining the type of soft tissue tumour. Where ever diagnosis was difficult or a differential diagnosis was made, ancillary study by immunohistochemistry was done to confirm the type. The primary antibodies and secondary detection system containing horse radish peroxides belonged to FDA approved company were used. The markers used in IHC were myogenin, EMA CK, CD99, chromogranin A CD31, S100, CD117, Desmin, Calretinin, Smooth muscle antigen and Vimentin. Approximately 3-4 mm tissue sections were taken in 3-Aminopropyl triethoxysilane coated slide along with control slide. The step was followed by deparaffinization in descending grades of alcohol, which was followed by antigen retrieval with TRIS buffer. Dedicated antigen retrieval (EZ-Retriever System v.3) was used for optimum retrieval of epitopes in a standardized laboratory condition. The non specific sites were blocked by peroxidase and power block inside a humidity chamber. Primary antibodies were incubated for duration of one hour. Finally secondary antibody, Super Enhancer Polymer-HRP and DAB chromogen was used in multiple steps. It was then counterstained with iron free hematoxylin.

The histopathological examination of all H and E stained slides were done as following:

  1. Identification of pattern of soft tissue
  2. Histological type of tumor (Benign or Malignant).
  3. Grading of tumor in case of malignancy.
  4. IHC done in selected cases of undifferentiated malignant tumors.

Results

The soft tissue tumors were classified based on WHO classification”. The relevant data’s were collected and recorded such as Age, Sex, Location of tumor and a final diagnosis were given with gross and microscopic characteristics. A total of 5895 cases were collected, out of which total 794 cases were noted to be a soft tissue tumors. In Table 1, Among 794 positive sample, 61 cases found to be malignant and rest cases was benign in nature. According to Table 2, the histological type, the most common type was found to be from Muscular tissues i.e 442 cases(55.7%), followed by vascular tissues i.e. 157 cases(19.8%) and Lipomatous tissues i.e 83 cases(10.4%).Incidence of Fibroblastic/My fibroblastic and Peripheral nerve sheath types were found to be almost equal. tumors have been mentioned. Soft tissue tumors were commonly seen in female gender (79.0%). Lipoma and hemangioma are most commonly seen in both genders. In the Table 3, some common types of benign and malignant soft tissue In Female most common benign tumor was leiomyoma followed by hemangioma, lipoma, fibroma, Nevus, schwanomma and neurofibroma while common malignant tumors was Rhabdomyosarcoma followed by synovial sarcoma.

Soft Tissue Tumor

Number of Cases

Percentage

Benign

733

92.8%

Malignant

61

7.60%

Total

794

100%

Table 1 Tumor according to the classification

Histological Type

Number of Cases

Percentage

Lipomatous tissues

83

10.40%

Fibroblastic/Myofibroblastic tissues

55

6.90%

Muscular tissues

442

55.70%

Peripheral nerve sheath

53

6.7%

Vascular tissues

157

19.80%

Miscellaneous

4

0.50%

Total

794

100

Table 2 Tumor according to histological type

Type of Tumor

Female

Male

Leiomyoma

408

02

Fibroma

25

19

Lipoma

42

38

Hemangioma

65

61

Nevus

11

07

Schwanomma

11

06

Neurofibroma

03

01

Giant cell tumor

02

02

Glomus tumor

03

00

Synovial sarcoma

03

00

Liposarcoma

01

02

Fibrosarcoma

02

05

Malignant fibrous histiocytoma

00

4

Rhabdomyosarcoma

03

3

Lieomyosarcoma

0

1

 

 

 

Dermatofibrosarcoma protuberance

01

00

Ganglioneuroblastoma

00

02

Malignant haemangioendothelioma

01

01

Percentage

79.00%

21.00%

Table 3 Tumor according to gender distribution

 In Male common benign tumor was Haemangioma followed by lipoma, Fibroma, Nevus and schwannoma while common malignant tumor was Fibrosarcoma followed by malignant fibrous histiocytoma, Rhabdomyosarcoma and Liposarcoma. In Table 4, as per the locations, Benign soft tissue tumors are commonly located in pelvis and Retroperitoneal sites (58.8%), among which uterus was the most common site, followed in decending order by Head and neck region (22.5%), Upper limb, Lower limb, Chest and Abdomen and Back region. Common site for Schwanomma and Neurofibroma, Giant cell tumor, Glomus tumor was Head and Neck and Upper limb respectively.

Among Malignant tumors Liposarcoma was commonly seen in Pelvis and Retro peritoneum followed by Fibrosarcoma in Chest and Abdomen region, malignant fibrous histiocytoma equally on Head and neck, upper limb, Chest and Abdomen and Back region. Rhabdomyosarcoma common site was Head and neck region, Ganglioneuroblastoma equally on Head and neck, Chest and Abdomen region. Synovial sarcoma equally on Head and Neck, Lower limb, Chest and Abdomen region and Malignant Hemangioendothelioma on Chest and Abdomen and Lower limb respectively. IHC was required mostly in diagnosis of malignant soft tissue tumours as adjunt to histology. The Common Markers used to differentiate sub-categorisation of Soft tissue tumors are shown in Table 5.

Type of Tumors

Head and Neck

Upper Limb

Lower Limb

Chest and Abdomen

Pelvis and Retroperitoneum

Back

Total

Leiomyoma

 

01

 

 

408

01

410

Fibroma

18

12

05

03

05

01

44

Lipoma

20

24

11

07

06

12

80

Hemangioma

101

15

07

01

01

01

126

Nevus

14

-

-

02

01

01

18

Schwanomma

05

01

01

04

04

02

17

Neurofibroma

-

02

01

-

01

-

04

Giant cell tumor

-

03

01

-

-

-

04

Glomus tumor

01

02

-

-

-

-

03

Synovial sarcoma

01

-

01

01

-

-

03

Liposarcoma

-

-

01

-

02

-

03

Fibrosarcoma

-

-

01

03

02

01

07

Malignant fibrous histiocytoma

01

01

-

1

-

01

4

Rhabdomyosarcoma

3

-

2

-

1

-

6

Leimyosarcoma

 

 

 

 

1

 

1

 

 

 

 

 

 

 

 

Dermatofibrosarcoma protuberance

-

-

01

-

-

-

01

Ganglioneuroblastoma

01

-

-

01

-

-

02

Malignant hemangioendothelioma

-

-

1

01

-

-

01

Percentage

22.50%

8.30%

4.40%

3.30%

58.80%

2.70%

100.00%

Table 4 Tumors according to locations

Tumors

Marker Positivity

Leiomyosarcoma

SMA+, Desmin +, Myogenin -

Liposarcoma

S100+, Vimentin+, Desmin-, Myogenin-

Fibrosarcoma

Vimentin+, Desmin-, Myogenin-

Rhabdomyosarcoma

Desmin+, Myogenin+, SMA-

Synovial Sarcoma

EMA+, Cytokeratin+,Vimentin+,BCL2+

Malignant Fibrous Histiocytoma

Vimentin+, Desmin-, EMA-

Dermatofibrosarcoma protuberance

CD34+, others -

Malignant hemangioendothelioma

CD34+, CD31+, Desmin -

Table 5 Immunohistochemistry in Malignant soft tissue tumors

Discussion

Enzinger F.M. & W.W. Weiss, Myhre Jenson et al.13 reported an incidence of soft tissue tumors as 0.8-1%, 0.8% and<2% respectively. This was the first study undertaken in this tertiary care institute on soft tissue tumour to describe patterns of soft tissue tumours. However the study was restricted to documentation the information about incidence, sex and site distribution of soft tissue tumors and confirming the morphological diagnosis with immunohistochemistry. Soft tissue tumors vary from most common benign Leiomyoma, Haemangioma, and Lipoma to some rare malignant ones. Thus incidence of benign tumor 12times more common than malignant in case of soft tissue tumors. We also encountered very rare types of malignant soft tissue tumour such as malignant hemangioendothelioma, granular cell tumour of tongue, Desmoblastic rhabdomyosarcoma etc.

Soft tissue tumors are diagnosed in Excisional biopsy of tumor mass and it is most appropriate method of diagnosis of Soft tissue tumors .The histological diagnosis and grading is mandatory as it has therapeutic and prognostic relevance.14 Among benign tumors Leiomyoma was most commonly seen in females and are very common in uterus followed by Hemangioma and lipoma, while in Male most common was Haemangioma followed by lipoma. Haemangioma are localized lesions confined to head and neck region while lipoma is usually painless soft mass common in neck, shoulder, lower limb and upper limb. Cases are more seen among females than males.

IHC was required mostly in diagnosis of malignant soft tissue tumours as adjunt to histology. Myogenin and Myo D1 were used for identifying origin of skeletal muscle origin. Similarly specific markers such CD31 was applied for blood vessel origin, S100 for shwannonian tumours and Liposarcoma, EMA for synovial sarcoma and MPNST and Vimentin for fibro sarcoma. Benign soft tissue tumors were more common than malignant tumors in our study, similar to the studies done by Angerwall et al.15 Enzinger, F.M.S.W. Weiss reported a benign to malignant ratio as 5:1 and 18.5 to 100:1 respectively.14–16 In present study benign to malignant ratio is 12:1

The general site distribution of benign soft tissue tumors site incidence as reported is 10% in head and neck region, 30% in Trunk, 20% in upper extremities, 40% in lower extremities. According to Natrajanm et al.17 & Costa J et al.18 the site distribution of benign soft tissue tumors was 4-9% in head & neck, 32% in trunk and 60-64% in extremities.17 In the present study the site distribution of soft tissue tumors was found to be 58.8% in pelvic and retroperitoneum, 22.5% in head & neck, 8.3% upper extremities, 4.4% lower extremities, 3.3% in chest and abdomen and 2.7% in back region. The rise in incidence of soft tissue tumors in Pelvis and Retroperitoneal region was due to the higher incidence of Leiomyoma followed by haemangiomas in Head and Neck region.

In our study benign soft tissue tumors were found more commonly in Females than males, observation made by Dev & Cotran reported an incidence of 58% in males, Costa j et al.18 reported an incidence of 55-60% in males.18,19 Mythre Jenson O et al.,13 Torjani et al.20 Tsuji Moto M et al.20 reported an incidence of 55-60% in males which in present study female sex incidence was found to be common 81%,19,20 while male sex incidence was found to be 19%. Haemangiomas were the second most common benign tumors and the common site was head and neck. Similar observations were made by Dev. Sex incidence of peripheral nerve tumors was observed to be more common in females in our study while studies done by Evans Enzinger FM Oberman & Sullenger 1967 show almost equal incidence.21,22

Glomus tumors occur in adults of all ages and sometimes in children, as per the study of Kohout & Stout.23 In the present study we had 2cases of glomus tumor constituting less than 1% of benign soft tissue tumors. In a review of 20 cases of Riversos & Pack 1950, 15cases (75%) occurred in the upper extremity, out of which 7cases(35%) were noticed subungually, 8cases (40%) occurred in lower extremity and 2cases (10%) in trunk & 1case(1%) in head & neck region. The site distribution in our study revealed that both the cases occurred in upper extremity (Figure 1). Present study showed 11cases of lymphangiomas found commonly in females. All of the cases occurred in head & neck region. This was similar to studies done by Willis 1967 and Watson & McCarthy 1940.

Figure 1 GLOMUS Tumor.

Weiss & Mentzel in their study of 46 and 24cases reported hemangioendothelioma in deep soft tissues. In our study we had only 2cases seen in Chest and Abdomen and lower limb region. Immunohistochemistry showed positivity for CD34 in our study. Fibrosarcoma comprise 5-10% of sarcomas according to Markhede G et al.24 In the study 7cases of fibro sarcomas were noted constituted an incidence of 24.1% of all soft tissue sarcomas. In a review of 695cases at AFIP 1970-79, 10% in head and neck, 17% trunk, 28% in upper extremities & 45% in lower extremities. Bizer LS 1971 noted a site distribution of 7.8% in head and neck, 51% in trunk, 17% in upper extremities & 23% in lower extremities.25 Hidayat AA26,27 and Enzinger FM & SW Weiss reported site distribution of 85-90% in extremities in which 50-60% was in lower extremity, 10-15% occurred in head and neck and trunk region. In our study most common site was Chest and Abdomen (trunk) followed by Pelvis and Retroperitoneal region. The incidence of liposarcoma reported by Costa J et al.18 was 10-25% among soft tissue sarcoma. In the present study 3cases were seen with an incidence 10.3% with male preponderance. Similar findings were found in studies done by AFIP, Reszel and Spittle Stout AP & Lattles R and Kindblomtt et al.15 reported a male preponderance. In present study all the cases showed positivity for S-100 (Figure 2).

Figure 2 LIPOSARCOMA.

Synovial sarcoma constitutes about 6-15% of all sarcomas as per Coasta J et al.18 In the present study the incidence was 10.3% of all soft tissue sarcomas. Studies by Mackenzie DH 1977, revealed M: F ratio to be 1.4:1 to 2:1, Cagle LA et al.27 reported roughly equal incidence in both sexes.27,28 In the present study 3cases were noted, all seen in Female. In a review of 141cases on the records of surgical pathology division of Columbia university revealed 61cases (43.3%) in lower extremities including 9cases in foot, 44cases (31.2%) in trunk and 13cases (9.2%) in head& neck region. Review by Leslie A et al.28 of 63cases, found lower extremities to be the common sites.29 In the present study there were 3cases which occurred in Lower extremity, Head and Neck and Chest and Abdomen region equally. In immunohistochemical study of 100 synovial sarcomas by Guillou et al. focal positivity for EMA and cytokeratin was found in 97% and 69% of cases. In present study, positivity for EMA and cytokeratin was seen.

In the study done by Anders Rydholm, out of 278 soft tissue sarcomas, 22% were malignant fibrous histiocytoma. Hashimoto H et al.,30 Costa j et al.18 & Lawrence et al.17 stated that 12-33% of soft tissue sarcomas were MFH.31 Present study shows an incidence of 13.8% of MFH out of all soft tissue sarcomas. Rooser B reported a sex incidence of M:F1.1:1. Obrein and Stout De Rosai & Lattes reported major site as in lower extremity & followed by chest wall, upper extremity and retroperitoneum. In the present study 4cases were noted with Male preponderence, with equal distribution on Head and Neck, Upper extremities, chest and Abdomen and Back region. In present study, out of four cases, one case of Malignant Fibrous Histiocytoma Giant cell type, a rare type was noted in 48 years old male patient. The Location of tumor was on abdominal wall. Immunohistochemistry was done which shows positivity for Vimentin and negative for Desmin and Cytokeratin (Figure 3-7). The existence of neoplasms bearing light microscopic features of giant cell tumor of bone (osteoclastoma) has been the focus of much attention and controversy in the literature. Such tumors were first described as a distinct pathologic entity by Rosai32 who reported two cases of this condition. Since then, ten additional cases have been added to the literature.33–40

Figure 3 MALIGNANT Fibrous Histocytoma Gaint Cell Type.

Figure 4 MALIGNANT fibrous histocytoma gaint cell type.

Figure 5 showing VIMENTIN positivity.

Figure 6 Showing DESMIN positivity.

Figure 7 CYTOKERATIN negativity.

Jeffrey reported another case in which ultrastructural examination failed to reveal epithelial features. The findings in their case, which in the opinion of the authors did not preclude an epithelial origin, more closely resembled those of giant cell tumor of bone. More recently, Manci et al.41 have described the ultrastructural features of an OGTP in which desmosomes and microvillus could not be identified, leading them to suggest that their case may be more closely related to extra skeletal osteoclastomas or to the giant cell type of malignant fibrous histiocytoma. Dimitris P, Agamandis in 1986 reported an incidence of Rhabdomyosarcoma as 19% of all soft tissue sarcoma. In the present study, we encountered 6cases of Rhabdomyosarcomas constituting an incidence of 20.7% of all soft tissue sarcomas. Out of 6cases one case was of embryonal rhabdomyosarcoma, which was positive for desmin, myogenin.

In present study out of 6cases, one case of Sclerosing Rhabdomyosarcoma was noted involving Head and Neck region (tongue), in 50years old male patient. Immunohistochemistry was done which shows strong positivity for Vimentin, weakly positivity for Desmin and 40% tumor cells positivity for Myogenin (Figure 8, Figure 9, Figure 10 & Figure 11). SRMS is an unusual variant of RMS that was first described in 2000 by Mentzel et al.42 They described three cases of RMS in adult patients, characterized by prominent hyaline sclerosis and a pseudo vascular growth pattern, and termed sclerosing, pseudo vascular rhabdomyosarcoma. In 2002, Folpe et al.43 also described four cases of an unusual hyalinizing, matrix-rich variant of RMS. They named it as sclerosing rhabdomyosarcoma.43 However, so far, there was still less than 40reported cases (the present case is not included) in English literatures.44–48 According to Julie. among the 39reported cases, SRMS can arise in a broad age ranged from 0.3 to 79years with an average age at 27. The most commonly involved sites (including the present case) are the extremities (19/40) and head and neck (16/40).48 Histological, SRMS has a characteristic constellation of features and is characterized by hyalinized, eosinophilic to basophilic matrix.49 Immunohistochemically, SRMS is usually strongly positive for Vimentin, Desmin and MyoD1, and weakly, focally positive for Moygenin suggesting its skeletal muscle differentiation, but negative for CK, S-100, CD34, and CD31.42,43,46,47

Gutierrez G et al.26 reported incidence of 1.1% of Dermatofibrosarcoma protruberance of all the soft tissue sarcomas and 0.06% of all malignant tumors.50 In the present study they constituted about 3.4% of all the soft tissue sarcomas. Gutierrez G et al.26 reported a male predominance accounting to 36%. Males are more frequently affected as reported by Enzinger FM & Weiss SW. In the present study a Female patient was involved. In a review of 853 cases at AFIP 1960-79 the site distribution was noted to be 14.5% in head and neck, 47.4% in trunk, 18.2% in upper extremities, and 19.9% in lower extremities. In the present study 1 case was noted in the lower extremity, which shows CD34 positivity. Only 1 case of Leiomyosarcomas was encountered in our study, constituting an incidence 3.4% of soft tissue sarcoma. The Location of tumor was Paratesticular region, a rare site in 71years old male patient. Immunohistochemistry shows strong positivity for SMA and Desmin, Moderately positivity for EMA and Vimentin and negative for S100 and Myogenin (Figures 12-14).

Figure 8 SCLEROSING Rahbdomyosarooma.

Figure 9 SCLEROSING rahbdomyosarooma.

Figure 10 Showing VIMENTIN positivity.

Figure 11 MYOGENIN positivity in 40% of tumor cells.

Figure 12 LEIOMYOSARCOMA showing SM actin.

Figure 13 Showing DESMIN positivity.

Figure 14 Showing DESMIN positivity.

Leiomyosarcomas of the genitourinary tract account for <5% of all sarcomas and <2% of all urological tumors. Approximately 100 paratesticular leiomyosarcomas have been reported in the literature. Leiomyosarcoma is a malignant soft tissue tumor that can arise from any tissue containing smooth muscle. However, leiomyosarcoma arising in paratesticular tissue is extremely rare and approximately only 10% of all paratesticular sarcomas are leiomyosarcomas.51 Paratesticular leiomyosarcoma originates from the spermatic cord, the scrotum, or the epididymis. The most common type is the spermatic cord type, which arises from undifferentiated mesenchymal cells of the cremasteric muscle and the vas deferens. The epididymal and scrotal types are less frequent and they originate from the smooth muscle surrounding the basement membrane of the epididymal canal and dartos layer, respectively.52 On immunohistochemical staining, expression of smooth muscle actin, muscle-specific actin and desmin is observed in most leiomyosarcomas, while expression of CD117, myogenin, Ki-67, S-100 protein and cytokeratin has also been reported in some cases.53

In present study 1 case of granular cell tumor (mixed Schwann cells and squamous cell origin) was found and was included in miscellaneous category. The tumor was found in Head and Neck region (Mandible), in 35years old Male patient. Immunohistochemistry shows positivity for S-100 and Cytokeratin and negative for Myogenin (Figures 15-19). GCTs are rare benign neoplasms, they may involve any organ of the body, about 50% of the tumors are found in the head and neck area.54,55 Granular cell tumors are more frequently found in adults, with rare occurrences in the pediatric population. Usually include benign tumors as they account for 98% of the cases.56 GCTs are almost always benign, but malignant manifestations are found in 1–2% of the patients. They are preferentially located in the skin and subcutaneous region. They involve the regional lymph nodes, although distal metastasis is uncommon. Malignancy is suspected from a series of factors.57 In immunohistochemistry granular cell tumors are positive for protein S-100 and neuron-specific enolase.

Figure 15 Granular cell tumor.

Figure 16 Granular cell tumor.

Figure 17 Showing S100 and CYTOKERATIN positivity.

Figure 18Showing S100 and CYTOKERATIN positivity.

Figure 19 MYOGENIN negativity.

Summary

Majority of the soft tissue tumors can be diagnosed by their individual characteristics on routine haematoxylin and eosin sections under light microscopy. Hence the light microscopy still remains as the basic method for the diagnosis of soft tissue tumors in majority of the institutes. Newer techniques such as cytogenetic, Immunocytochemistry and electron microscopic study being widely used diagnostic tools to solve the difficult cases of soft tissue tumors. Although these methods are more reliable, their high cost is the major drawback. Immunocytochemical methods also have a limitation of significant overlapping in their findings among different soft tissue tumors and no single marker alone can reliably be used to substantiate the presumptive diagnosis. In the “Histomorphology study of soft tissue tumors” total 5895 cases were reviewed, out of which 794cases were soft tissue origin. Majority of which were benign with the ratio of 12:1 Histological most common benign tumor among females was leiomyoma followed by haemangioma and lipoma and common malignant were Rhabdomyosarcoma and synovial sarcoma. While in male common benign was Haemangioma followed by lipoma and common malignant was Fibrosarcoma followed by Rhabdomyosarcoma.

Acknowledgements

None.

Conflict of interest

The author declares no conflict of interest.

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