An immunohistochemical atlas of necroptotic pathway expression

坏死性凋亡通路表达的免疫组织化学图谱

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作者:Shene Chiou # ,Aysha H Al-Ani # ,Yi Pan ,Komal M Patel ,Isabella Y Kong ,Lachlan W Whitehead ,Amanda Light ,Samuel N Young ,Marilou Barrios ,Callum Sargeant ,Pradeep Rajasekhar ,Leah Zhu ,Anne Hempel ,Ann Lin ,James A Rickard ,Cathrine Hall ,Pradnya Gangatirkar ,Raymond Kh Yip ,Wayne Cawthorne ,Annette V Jacobsen ,Christopher R Horne ,Katherine R Martin ,Lisa J Ioannidis ,Diana S Hansen ,Jessica Day ,Ian P Wicks ,Charity Law ,Matthew E Ritchie ,Rory Bowden ,Joanne M Hildebrand ,Lorraine A O'Reilly ,John Silke ,Lisa Giulino-Roth ,Ellen Tsui ,Kelly L Rogers ,Edwin D Hawkins ,Britt Christensen ,James M Murphy ,André L Samson

Abstract

Necroptosis is a lytic form of regulated cell death reported to contribute to inflammatory diseases of the gut, skin and lung, as well as ischemic-reperfusion injuries of the kidney, heart and brain. However, precise identification of the cells and tissues that undergo necroptotic cell death in vivo has proven challenging in the absence of robust protocols for immunohistochemical detection. Here, we provide automated immunohistochemistry protocols to detect core necroptosis regulators - Caspase-8, RIPK1, RIPK3 and MLKL - in formalin-fixed mouse and human tissues. We observed surprising heterogeneity in protein expression within tissues, whereby short-lived immune barrier cells were replete with necroptotic effectors, whereas long-lived cells lacked RIPK3 or MLKL expression. Local changes in the expression of necroptotic effectors occurred in response to insults such as inflammation, dysbiosis or immune challenge, consistent with necroptosis being dysregulated in disease contexts. These methods will facilitate the precise localisation and evaluation of necroptotic signaling in vivo. Keywords: IBD; Immunohistochemistry; MLKL; Necroptosis; RIPK3.

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