Hepatic fibropoiesis in dogs naturally infected with Leishmania (Leishmania) infantum treated with liposome-encapsulated meglumine antimoniate and allopurinol

IF 2.2 2区农林科学 Q2 PARASITOLOGY Veterinary parasitology Pub Date : 2018-01-30 DOI:10.1016/j.vetpar.2017.12.005

R.S. Castro , I.F.G. de Amorim , R.A. Pereira , S.M. Silva , L.J. Pinheiro , A.J.W. Pinto , E.G. Azevedo , C. Demicheli , M.M.V. Caliari , D.M. Mosser , M.S.M. Michalick , Frédéric J.G. Frezard , Wagner L. Tafuri

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引用次数: 7

Abstract

Hepatic fibropoiesis in canine visceral leishmaniasis (CVL) were evaluated by histological (morphometrical collagen deposition) and immunohistochemical assays characterizing alpha-actin (α-SMA), vimentin, calprotectin (L1 antigen), and TGF-β in 46 naturally infected dogs with Leishmania infantum treated with liposome-encapsulated meglumine antimoniate and allopurinol separately and in combination. Six treatment groups were defined: meglumine antimoniate encapsulated in nanometric liposomes (LMA), allopurinol (ALLOP); liposome-encapsulated meglumine antomoniate combined with allopurinol (LMA + ALLOP); empty liposomes (LEMP); empty liposomes combined with allopurinol (LEMP + ALLOP) and saline. Relative liver weight was lower in LMA, LMA + ALLOP, and ALLOP groups compared to the LEMP control. Significantly lower granulomatous chronic inflammatory reaction was seen in the ALLOP group compared to a control group. Calprotectin was lowest in liver of those dogs showing lower numbers of intralobular hepatic granulomas. Collagen deposits were significantly higher in LMA compared to ALLOP, LEMP + ALLOP, and Saline groups. LMA + ALLOP group collagen deposition was higher than dogs treated only with allopurinol. Immunohistochemical analysis showed significant higher α-SMA in hepatic stellate cells (HSCs), hepatic perisinusoidal cells, in control groups than LMA + ALLOP and LEMP + ALLOP. Alpha-actin and Vimentin positive cells were diffusely distributed throughout the liver parenchyma in the hepatic lobule, mainly in HSCs. Vimentin expression was significantly higher in the saline group than in the ALLOP group. Our data suggest that allopurinol inhibits HSC and results in lower collagen deposits in liver during CVL progression, as supported by the significantly lower expression of TGF-β in the ALLOP group compared to other groups. Results demonstrated that treatment with allopurinol inhibited chronic granulomatous inflammatory reaction and hepatic fibrosis in CVL.

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用脂粒包埋的锑酸三聚氰胺和别嘌呤醇治疗自然感染利什曼原虫(利什曼原虫)婴儿的狗的肝纤维化

本文对46只自然感染利什曼病的犬分别或联合给予脂脂包封的氨酸甲氨胺和别嘌呤醇治疗，采用组织学(形态测量性胶原沉积)和免疫组化检测α-肌动蛋白(α-SMA)、vimentin、钙保护蛋白(L1抗原)和TGF-β，评价犬内脏利什曼病(CVL)的肝纤维化情况。确定了六个治疗组:包封在纳米脂质体(LMA)中的锑酸甲氨胺、别嘌呤醇(ALLOP);脂质体包封的异嘌呤醇联合异嘌呤醇(LMA + ALLOP);空脂质体(LEMP);空脂质体联合别嘌呤醇(LEMP + ALLOP)和生理盐水。与LEMP对照组相比，LMA组、LMA + ALLOP组和ALLOP组的相对肝脏重量较低。与对照组相比，ALLOP组肉芽肿性慢性炎症反应明显降低。肝小叶内肉芽肿数量较少的狗，其肝脏钙保护蛋白含量最低。与ALLOP组、LEMP + ALLOP组和生理盐水组相比，LMA中的胶原沉积明显增加。LMA + ALLOP组胶原沉积高于单纯别嘌呤醇组。免疫组化分析显示，对照组肝星状细胞(hsc)、肝周围细胞α-SMA含量明显高于LMA + ALLOP和LEMP + ALLOP。α -肌动蛋白和Vimentin阳性细胞广泛分布于肝小叶的肝实质，主要分布在造血干细胞中。生理盐水组Vimentin表达明显高于ALLOP组。我们的数据表明，别嘌呤醇抑制HSC，导致CVL进展过程中肝脏胶原沉积减少，与其他组相比，ALLOP组中TGF-β的表达显著降低。结果表明，别嘌呤醇治疗可抑制CVL的慢性肉芽肿炎症反应和肝纤维化。

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来源期刊

Veterinary parasitology 农林科学-寄生虫学

CiteScore

5.30

自引率

7.70%

发文量

126

审稿时长

36 days

期刊介绍： The journal Veterinary Parasitology has an open access mirror journal,Veterinary Parasitology: X, sharing the same aims and scope, editorial team, submission system and rigorous peer review. This journal is concerned with those aspects of helminthology, protozoology and entomology which are of interest to animal health investigators, veterinary practitioners and others with a special interest in parasitology. Papers of the highest quality dealing with all aspects of disease prevention, pathology, treatment, epidemiology, and control of parasites in all domesticated animals, fall within the scope of the journal. Papers of geographically limited (local) interest which are not of interest to an international audience will not be accepted. Authors who submit papers based on local data will need to indicate why their paper is relevant to a broader readership. Parasitological studies on laboratory animals fall within the scope of the journal only if they provide a reasonably close model of a disease of domestic animals. Additionally the journal will consider papers relating to wildlife species where they may act as disease reservoirs to domestic animals, or as a zoonotic reservoir. Case studies considered to be unique or of specific interest to the journal, will also be considered on occasions at the Editors'' discretion. Papers dealing exclusively with the taxonomy of parasites do not fall within the scope of the journal.