Association of tumour-infiltrating regulatory T cells with adverse outcomes in dogs with malignant tumours
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Sakai, K.
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Univ Tokyo, Grad Sch Agr & Life Sci, Dept Vet Clin Pathobiol, Tokyo, JapanUniv Tokyo, Grad Sch Agr & Life Sci, Dept Vet Clin Pathobiol, Tokyo, Japan
Sakai, K.
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Maeda, S.
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Yamada, Y.
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Univ Tokyo, Grad Sch Agr & Life Sci, Dept Vet Clin Pathobiol, Tokyo, JapanUniv Tokyo, Grad Sch Agr & Life Sci, Dept Vet Clin Pathobiol, Tokyo, Japan
Yamada, Y.
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Chambers, J. K.
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Univ Tokyo, Grad Sch Agr & Life Sci, Dept Vet Pathol, Tokyo, JapanUniv Tokyo, Grad Sch Agr & Life Sci, Dept Vet Clin Pathobiol, Tokyo, Japan
Chambers, J. K.
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Uchida, K.
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Nakayama, H.
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Univ Tokyo, Grad Sch Agr & Life Sci, Dept Vet Pathol, Tokyo, JapanUniv Tokyo, Grad Sch Agr & Life Sci, Dept Vet Clin Pathobiol, Tokyo, Japan
Nakayama, H.
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Yonezawa, T.
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Univ Tokyo, Grad Sch Agr & Life Sci, Dept Vet Clin Pathobiol, Tokyo, JapanUniv Tokyo, Grad Sch Agr & Life Sci, Dept Vet Clin Pathobiol, Tokyo, Japan
Yonezawa, T.
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Matsuki, N.
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Univ Tokyo, Grad Sch Agr & Life Sci, Dept Vet Clin Pathobiol, Tokyo, JapanUniv Tokyo, Grad Sch Agr & Life Sci, Dept Vet Clin Pathobiol, Tokyo, Japan
Matsuki, N.
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[1] Univ Tokyo, Grad Sch Agr & Life Sci, Dept Vet Clin Pathobiol, Tokyo, Japan
[2] Univ Tokyo, Grad Sch Agr & Life Sci, Dept Vet Pathol, Tokyo, Japan
Regulatory T cells (Tregs) infiltrate into a variety of tumour tissues and associate with poor prognosis in humans. However, data on association of Treg infiltration with prognosis is limited in canine tumours. The purpose of this study was to examine the number of tumour-infiltrating Tregs and its association with overall survival (OS) in dogs with malignant tumours. The following 168 canine tumours were included: 37 oral malignant melanomas (OMMs); 14 oral squamous cell carcinomas (OSCCs); 16 pulmonary adenocarcinomas (PAs); 37 mammary carcinomas (MCs); 36 mast cell tumours (MCTs) and 28 hepatocellular carcinomas (HCCs). Normal tissues were obtained from 8 healthy dogs as controls. The number of forkhead box P3 (Foxp3)-positive Tregs in intratumoral and peritumoral areas was investigated by immunohistochemistry. OS was compared between high and low Treg groups. The number of intratumoral and peritumoral Foxp3-positive Tregs was significantly higher in OMM, OSCC, PA and MC compared with each normal tissue. There were few Foxp3-positive Tregs in MCT and HCC. With intratumoral Tregs, the OS in the high Treg group was significantly shorter than that in the low Treg group in OMM, OSCC and PA. With peritumoral Tregs, there was no significant difference for OS between the 2 groups in each tumour type. These results suggest that Tregs infiltrate into a variety of canine tumours and the abundance of Tregs are associated with poor prognosis in some solid tumour types.