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Alveolar soft part sarcoma

October 25, 2023

Alveolar soft part sarcoma, abbreviated ASPS, is a very rare type of soft-tissue sarcoma, that grows slowly and whose cell of origin is unknown.

Alveolar soft part sarcoma
Other namesAlveolar soft-tissue sarcoma
Micrograph of an alveolar soft part sarcoma, showing the characteristic alveolar-like architecture and cells with eccentric nuclei and abundant eosinophilic cytoplasm. H&E stain.
SpecialtyOncology 

ASPS arises mainly in children and young adults and can migrate (metastasize) into other parts of the body, typically the lungs and the brain. Typically, ASPS arises in muscles and deep soft tissue of the thigh or the leg (lower extremities), but can also appear in the upper extremities (hands, neck, and head). While ASPS is a soft tissue sarcoma, it can also spread and grow inside the bones.

Etymology Edit

  • The term alveolar comes from the microscopic pattern, visible during the analysis of slides of ASPS under the microscope in histopathology. The tumor cells seem to be arranged in the same pattern as the cells of the small air sacks (alveoli) in the lungs. However, this is just a structural similarity. ASPS was first described and characterized in 1952.[1]
  • ASPS is a sarcoma, and that indicates that this cancer initially arises from tissue of embryonic mesenchymal origin. (The fertilized egg divides and redivides forming a sphere. Early in embryogenesis, dimples appear in the poles of the sphere and burrow through the sphere forming an inner passage that will ultimately form the gut. Malignancies arising from cells that were originally part of the outer layer of the sphere and those that were part of the embryonic tunnel are termed carcinomas; malignancies arising from the cells between the outer layer and the inner burrow are termed sarcomas.)

Causes Edit

Chromosomal analysis of ASPS shows the breaking and joining of two chromosomes in the tumor cells. A piece of chromosome X breaks and is joined to chromosome 17.[2] This translocation creates a fusion between two genes named ASPL and TFE3, which results in the formation of an aberrant protein (termed fusion protein) that is not found in normal cells. Two sorts of fusions between chromosome X and chromosome 17 are found in different ASPS tumors: type one and type two.

Dr. Marc Ladanyi at Memorial Sloan-Kettering Cancer Center, in New York City, has pioneered this work. The resultant fusion protein ASPLTFE3 is a rogue transcription factor that is the driver of aberrant cellular behavior including uncontrolled cell division and enhanced angiogenesis.

Diagnosis Edit

 
High-magnification micrograph showing the characteristic large cells with abundant eosinophilic, i.e. pink, cytoplasm and an eccentrically placed nucleus. H&E stain.

ASPS may exist in the patient’s body for a long time before being diagnosed. It can grow large and push aside surrounding tissues for a long time before causing any discomfort. Therefore, ASPS symptoms may either be a painless swelling, or a soreness caused by compressed nerves or muscles, affecting the range of motion in the area.

Pathology Edit

The definitive diagnosis of ASPS is based on its appearance under the microscope (i.e., its histomorphology), and presence of the characteristic chromosomal translocation (i.e., cytogenetics).

ASPS' histomorphologic features include an alveolar-like pattern at low magnification and the presence of large cells with abundant eosinophilic cytoplasm and eccentric nuclei. Calcifications are commonly present, as may be seen with slow-growing neoplasms.

Prognosis Edit

Although ASPS displays a relatively indolent course, the ultimate prognosis is poor and is often characterized by late metastases.[3]

Epidemiology Edit

ASPS is an extremely rare cancer. While sarcomas comprise about 1% of all newly diagnosed cancers, and 15% of all childhood cancers, ASPS comprises less than 1% of sarcomas. According to the American Cancer Society, about 9530 new cases of soft tissue sarcoma will be diagnosed in the USA in 2006. This predicts under 100 new cases of ASPS. Such low numbers of occurrence seriously impede the search for a cure by making it hard to gather any meaningful statistics about the disease. As a result, finding the best treatment option often involves making a lot of educated guesses.

Research Edit

  • In terms of origin, it was recently demonstrated that although ASPS generally arises in muscle tissue, the cells do not express muscle markers at the mRNA level and more closely resemble mesenchymal stromal cells.[10]

References Edit

  1. ^ Christopherson WM, Foote FW, Stewart FW (1952). "Alveolar soft part sarcomas: structurally characteristic tumors of uncertain histogenesis". Cancer. 1952 (5): 100–111. doi:10.1002/1097-0142(195201)5:1<100::aid-cncr2820050112>3.0.co;2-k. PMID 14886902.
  2. ^ Ladanyi M, Lui MY, Antonescu CR, Krause-Boehm A, Meindl A, Argani P, et al. (January 2001). "The der(17)t(X;17)(p11;q25) of human alveolar soft part sarcoma fuses the TFE3 transcription factor gene to ASPL, a novel gene at 17q25". Oncogene. 20 (1): 48–57. doi:10.1038/sj.onc.1204074. PMID 11244503.
  3. ^ Shelke P, Sarode GS, Sarode SC, Anand R, Prajapati G, Patil S (2018). "Alveolar soft-part sarcoma of the oral cavity: A review of literature". Rare Tumors. 10: 2036361318810907. doi:10.1177/2036361318810907. PMC 6299302. PMID 30574289.
  4. ^ Vistica DT, Hollingshead M, Borgel SD, Kenney S, Stockwin LH, Raffeld M, et al. (August 2009). "Therapeutic vulnerability of an in vivo model of alveolar soft part sarcoma (ASPS) to antiangiogenic therapy". Journal of Pediatric Hematology/Oncology. 31 (8): 561–70. doi:10.1097/MPH.0b013e3181a6e043. PMC 2784654. PMID 19636271.
  5. ^ Kenney S, Vistica DT, Stockwin LH, Burkett S, Hollingshead MG, Borgel SD, et al. (July 2011). "ASPS-1, a novel cell line manifesting key features of alveolar soft part sarcoma". Journal of Pediatric Hematology/Oncology. 33 (5): 360–8. doi:10.1097/MPH.0b013e3182002f9f. PMC 7518051. PMID 21552147. S2CID 25794748.
  6. ^ Tsuda M, Davis IJ, Argani P, Shukla N, McGill GG, Nagai M, et al. (February 2007). "TFE3 fusions activate MET signaling by transcriptional up-regulation, defining another class of tumors as candidates for therapeutic MET inhibition". Cancer Research. 67 (3): 919–29. doi:10.1158/0008-5472.CAN-06-2855. PMID 17283122.
  7. ^ Kummar S, Allen D, Monks A, Polley EC, Hose CD, Ivy SP, et al. (June 2013). "Cediranib for metastatic alveolar soft part sarcoma". Journal of Clinical Oncology. 31 (18): 2296–302. doi:10.1200/JCO.2012.47.4288. PMC 3677840. PMID 23630200.
  8. ^ Brahmi M, Vanacker H, Dufresne A (July 2020). "Novel therapeutic options for alveolar soft part sarcoma: antiangiogenic therapy, immunotherapy and beyond". Current Opinion in Oncology. 32 (4): 295–300. doi:10.1097/CCO.0000000000000652. PMID 32541316.
  9. ^ Goodwin ML, Jin H, Straessler K, Smith-Fry K, Zhu JF, Monument MJ, et al. (December 2014). "Modeling alveolar soft part sarcomagenesis in the mouse: a role for lactate in the tumor microenvironment". Cancer Cell. 26 (6): 851–862. doi:10.1016/j.ccell.2014.10.003. PMC 4327935. PMID 25453902.
  10. ^ Stockwin LH (2020-06-19). "Alveolar soft-part sarcoma (ASPS) resembles a mesenchymal stromal progenitor: evidence from meta-analysis of transcriptomic data". PeerJ. 8: e9394. doi:10.7717/peerj.9394. PMC 7307565. PMID 32596059.

External links Edit

October 25, 2023
alveolar, soft, part, sarcoma, abbreviated, asps, very, rare, type, soft, tissue, sarcoma, that, grows, slowly, whose, cell, origin, unknown, other, namesalveolar, soft, tissue, sarcomamicrograph, alveolar, soft, part, sarcoma, showing, characteristic, alveola. Alveolar soft part sarcoma abbreviated ASPS is a very rare type of soft tissue sarcoma that grows slowly and whose cell of origin is unknown Alveolar soft part sarcomaOther namesAlveolar soft tissue sarcomaMicrograph of an alveolar soft part sarcoma showing the characteristic alveolar like architecture and cells with eccentric nuclei and abundant eosinophilic cytoplasm H amp E stain SpecialtyOncology ASPS arises mainly in children and young adults and can migrate metastasize into other parts of the body typically the lungs and the brain Typically ASPS arises in muscles and deep soft tissue of the thigh or the leg lower extremities but can also appear in the upper extremities hands neck and head While ASPS is a soft tissue sarcoma it can also spread and grow inside the bones Contents 1 Etymology 2 Causes 3 Diagnosis 3 1 Pathology 4 Prognosis 5 Epidemiology 6 Research 7 References 8 External linksEtymology EditThe term alveolar comes from the microscopic pattern visible during the analysis of slides of ASPS under the microscope in histopathology The tumor cells seem to be arranged in the same pattern as the cells of the small air sacks alveoli in the lungs However this is just a structural similarity ASPS was first described and characterized in 1952 1 ASPS is a sarcoma and that indicates that this cancer initially arises from tissue of embryonic mesenchymal origin The fertilized egg divides and redivides forming a sphere Early in embryogenesis dimples appear in the poles of the sphere and burrow through the sphere forming an inner passage that will ultimately form the gut Malignancies arising from cells that were originally part of the outer layer of the sphere and those that were part of the embryonic tunnel are termed carcinomas malignancies arising from the cells between the outer layer and the inner burrow are termed sarcomas Causes EditChromosomal analysis of ASPS shows the breaking and joining of two chromosomes in the tumor cells A piece of chromosome X breaks and is joined to chromosome 17 2 This translocation creates a fusion between two genes named ASPL and TFE3 which results in the formation of an aberrant protein termed fusion protein that is not found in normal cells Two sorts of fusions between chromosome X and chromosome 17 are found in different ASPS tumors type one and type two Dr Marc Ladanyi at Memorial Sloan Kettering Cancer Center in New York City has pioneered this work The resultant fusion protein ASPL TFE3 is a rogue transcription factor that is the driver of aberrant cellular behavior including uncontrolled cell division and enhanced angiogenesis Diagnosis Edit nbsp High magnification micrograph showing the characteristic large cells with abundant eosinophilic i e pink cytoplasm and an eccentrically placed nucleus H amp E stain ASPS may exist in the patient s body for a long time before being diagnosed It can grow large and push aside surrounding tissues for a long time before causing any discomfort Therefore ASPS symptoms may either be a painless swelling or a soreness caused by compressed nerves or muscles affecting the range of motion in the area Pathology Edit The definitive diagnosis of ASPS is based on its appearance under the microscope i e its histomorphology and presence of the characteristic chromosomal translocation i e cytogenetics ASPS histomorphologic features include an alveolar like pattern at low magnification and the presence of large cells with abundant eosinophilic cytoplasm and eccentric nuclei Calcifications are commonly present as may be seen with slow growing neoplasms Prognosis EditAlthough ASPS displays a relatively indolent course the ultimate prognosis is poor and is often characterized by late metastases 3 Epidemiology EditASPS is an extremely rare cancer While sarcomas comprise about 1 of all newly diagnosed cancers and 15 of all childhood cancers ASPS comprises less than 1 of sarcomas According to the American Cancer Society about 9530 new cases of soft tissue sarcoma will be diagnosed in the USA in 2006 This predicts under 100 new cases of ASPS Such low numbers of occurrence seriously impede the search for a cure by making it hard to gather any meaningful statistics about the disease As a result finding the best treatment option often involves making a lot of educated guesses Research EditThe first xenograft model of ASPS for type one was established in mice by David Vistica at the National Cancer Institute in Frederick MD in 2009 4 The same authors subsequently generated the first publicly available ASPS cell line designated ASPS 1 5 An important advance involved demonstrating that the ASPL TFE3 fusion protein a transcription factor enhanced expression of the receptor tyrosine kinase c MET making ASPS sensitive to small molecule kinase inhibitor such as sunitinib 6 7 Current clinical trials are exploring the utility of kinase inhibitors targeting growth factor pathways and angiogenesis checkpoint inhibitors and cellular immunotherapies in the treatment of ASPS 8 Researchers at the Huntsman Cancer Institute HCI in Utah demonstrated that ASPS might be driven in part by lactate both being used as a fuel and driving angiogenesis 9 In terms of origin it was recently demonstrated that although ASPS generally arises in muscle tissue the cells do not express muscle markers at the mRNA level and more closely resemble mesenchymal stromal cells 10 References Edit Christopherson WM Foote FW Stewart FW 1952 Alveolar soft part sarcomas structurally characteristic tumors of uncertain histogenesis Cancer 1952 5 100 111 doi 10 1002 1097 0142 195201 5 1 lt 100 aid cncr2820050112 gt 3 0 co 2 k PMID 14886902 Ladanyi M Lui MY Antonescu CR Krause Boehm A Meindl A Argani P et al January 2001 The der 17 t X 17 p11 q25 of human alveolar soft part sarcoma fuses the TFE3 transcription factor gene to ASPL a novel gene at 17q25 Oncogene 20 1 48 57 doi 10 1038 sj onc 1204074 PMID 11244503 Shelke P Sarode GS Sarode SC Anand R Prajapati G Patil S 2018 Alveolar soft part sarcoma of the oral cavity A review of literature Rare Tumors 10 2036361318810907 doi 10 1177 2036361318810907 PMC 6299302 PMID 30574289 Vistica DT Hollingshead M Borgel SD Kenney S Stockwin LH Raffeld M et al August 2009 Therapeutic vulnerability of an in vivo model of alveolar soft part sarcoma ASPS to antiangiogenic therapy Journal of Pediatric Hematology Oncology 31 8 561 70 doi 10 1097 MPH 0b013e3181a6e043 PMC 2784654 PMID 19636271 Kenney S Vistica DT Stockwin LH Burkett S Hollingshead MG Borgel SD et al July 2011 ASPS 1 a novel cell line manifesting key features of alveolar soft part sarcoma Journal of Pediatric Hematology Oncology 33 5 360 8 doi 10 1097 MPH 0b013e3182002f9f PMC 7518051 PMID 21552147 S2CID 25794748 Tsuda M Davis IJ Argani P Shukla N McGill GG Nagai M et al February 2007 TFE3 fusions activate MET signaling by transcriptional up regulation defining another class of tumors as candidates for therapeutic MET inhibition Cancer Research 67 3 919 29 doi 10 1158 0008 5472 CAN 06 2855 PMID 17283122 Kummar S Allen D Monks A Polley EC Hose CD Ivy SP et al June 2013 Cediranib for metastatic alveolar soft part sarcoma Journal of Clinical Oncology 31 18 2296 302 doi 10 1200 JCO 2012 47 4288 PMC 3677840 PMID 23630200 Brahmi M Vanacker H Dufresne A July 2020 Novel therapeutic options for alveolar soft part sarcoma antiangiogenic therapy immunotherapy and beyond Current Opinion in Oncology 32 4 295 300 doi 10 1097 CCO 0000000000000652 PMID 32541316 Goodwin ML Jin H Straessler K Smith Fry K Zhu JF Monument MJ et al December 2014 Modeling alveolar soft part sarcomagenesis in the mouse a role for lactate in the tumor microenvironment Cancer Cell 26 6 851 862 doi 10 1016 j ccell 2014 10 003 PMC 4327935 PMID 25453902 Stockwin LH 2020 06 19 Alveolar soft part sarcoma ASPS resembles a mesenchymal stromal progenitor evidence from meta analysis of transcriptomic data PeerJ 8 e9394 doi 10 7717 peerj 9394 PMC 7307565 PMID 32596059 External links Edit Retrieved from https en wikipedia org w index php title Alveolar soft part sarcoma amp oldid 1170002848, wikipedia, wiki, book, books, library,

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