Evaluation and comparison of outcomes in dogs with periarticular and nonperiarticular histiocytic sarcoma

Klahn, Shawna; Kitchell, Barbara E.; Dervisis, Nikolaos

doi:10.2460/javma.239.1.90

Cited by 58 publications

(93 citation statements)

References 7 publications

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“…72 Early detection and treatment of articular HS is potentially curative, while disseminated HS has a worse prognosis. 5,34 However, articular HS is capable of widespread dissemination since histiocytes, especially those of the various DC lineages, are actively migratory cells. This is reflected in the median survival of dogs with articular HS and evidence of metastatic disease (about 5-8 months).…”

Section: Distinctive Histiocytic Sarcoma Syndromesmentioning

confidence: 99%

“…This is reflected in the median survival of dogs with articular HS and evidence of metastatic disease (about 5-8 months). 18,34 Articular HS has a distinctive appearance: it occurs as multiple tan nodules located beneath the synovial lining. Hence, these lesions begin outside of the synovial space either within the joint and/or in a periarticular location.…”

Section: Distinctive Histiocytic Sarcoma Syndromesmentioning

confidence: 99%

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A Review of Histiocytic Diseases of Dogs and Cats

2014

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Histiocytic proliferative disorders are commonly observed in dogs and less often cats. Histiocytic disorders occur in most of the dendritic cell (DC) lineages. Canine cutaneous histiocytoma originates from Langerhans cells (LCs) indicated by expression of CD1a, CD11c/CD18, and E-cadherin. When histiocytomas occur as multiple lesions in skin with optional metastasis to lymph nodes and internal organs, the disease resembles cutaneous Langerhans cell histiocytosis of humans. Langerhans cell disorders do not occur in feline skin. Feline pulmonary LCH has been recognized as a cause of respiratory failure due to diffuse pulmonary infiltration by histiocytes, which express CD18 and E-cadherin and contain Birbeck's granules. In dogs and cats, histiocytic sarcomas (HS) arise from interstitial DCs that occur in most tissues of the body. Histiocytic sarcomas begin as localized lesions, which rapidly disseminate to many organs. Primary sites include spleen, lung, skin, brain (meninges), lymph node, bone marrow, and synovial tissues of limbs. An indolent form of localized HS, progressive histiocytosis, originates in the skin of cats. Hemophagocytic HS originates in splenic red pulp and bone marrow macrophages in dogs and cats. In dogs, histiocytes in hemophagocytic HS express CD11d/CD18, which is a leuko-integrin highly expressed by macrophages in splenic red pulp and bone marrow. Canine reactive histiocytic diseases, systemic histiocytosis (SH) and cutaneous histiocytosis, are complex inflammatory diseases with underlying immune dysregulation. The lesions are dominated by activated interstitial DCs and lymphocytes, which invade vessel walls and extend as vasocentric infiltrates in skin, lymph nodes, and internal organs (SH).

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Section: Distinctive Histiocytic Sarcoma Syndromesmentioning

confidence: 99%

Section: Distinctive Histiocytic Sarcoma Syndromesmentioning

confidence: 99%

A Review of Histiocytic Diseases of Dogs and Cats

2014

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“…Dogs with HS (hereafter referred to as HS dogs) exhibit generally poor treatment outcomes because of the tumor's aggressive biological behavior, including its high cell proliferation, multidrug resistance, and metastatic potential (Yamazaki et al, 2013(Yamazaki et al, , 2014. Lomustine (CCNU) or doxorubicin have been commonly used as antitumor agents for HS dogs (Rassnick et al, 2010); however, the therapeutic benefit on the disseminated and hemophagocytic HS is insufficient because of resistance to these drugs (Klahn et al, 2011;Rassnick et al, 2010). It is suggested that overexpression of the inhibitor of apoptosis protein (IAP) and P-glycoprotein (P-gp) is able to induce multidrug resistance in breast cancer cells and its chemoresistant cells (Liu et al, 2007.…”

Section: Introductionmentioning

confidence: 99%

Survivin suppressor (YM155) enhances chemotherapeutic efficacy against canine histiocytic sarcoma in murine transplantation models

Yamazaki

Takagi

Hosoya

et al. 2015

Research in Veterinary Science

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“…Prognosis depends on the location of primary lesions: splenic HS commonly shows poor prognosis, whereas periarticular HS shows a better prognosis compared with non-periarticular HS (Klahn et al, 2011). We have shown that non-periarticular HS dogs exhibited significantly higher survivin expression, shorter DFI and ST as compared with other periarticular HS.…”

Section: Discussionmentioning

confidence: 73%

“…Response to CCNU was assessed based on diagnostic imaging of the chest, abdomen, and each primary location according to previously reported procedures (Klahn et al, 2011) and classified as follows: (1) complete response (disappearance of all clinical signs and disease through to at least day 21); (2) partial response (>50% or <100% decreases through to at least day 21); (3) stable disease (≤50% decreases or <20% increases through to at least day 21), or (4) progressive disease (≥20% increases in tumor volume or the development of new neoplastic lesions or metastases).…”

Section: Disease Free Interval and Survival Time In Test Casesmentioning

confidence: 99%