Hepatocyte entry leads to degradation of autoreactive CD8 T cells

Benseler, Volker; Warren, Alessandra; Vo, Michelle; Holz, Lauren E.; Tay, Szun S.; Couteur, David G. Le; Breen, Edmond J.; Allison, A. C.; Rooijen, Nico van; McGuffog, Claire; Schlitt, Hans J.; Bowen, David G.; McCaughan, Geoffrey W.; Bertolino, Patrick

doi:10.1073/pnas.1112251108

Cited by 141 publications

(147 citation statements)

References 32 publications

(33 reference statements)

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“…Regardless of de novo (rAAV.K b treatment in this study) or transgenic [Alb-K b mice (8,13,17,25)] expression, Des T cells activated by hepatocytes never developed into CTL, a finding similarly observed for OT-I T cells activated intrahepatically by de novo-expressed loweraffinity ligands. Overall, a wide variety of outcomes have been reported after intrahepatic CD8 T-cell activation in mice expressing transgenic liver antigens, including ignorance (33), deletional tolerance (8,13,17,25), and partial or full effector differentiation (11,12,24,34). These variable outcomes are likely caused by the different TCR:pMHC affinity and/or levels of antigen expression in these models.…”

Section: Discussionsupporting

confidence: 67%

“…First, this study ends an ongoing debate over whether T-cell tolerance observed in transgenic models is primarily a result of central tolerance or other regulatory mechanisms caused by constitutive transgene expression (11,12). Regardless of de novo (rAAV.K b treatment in this study) or transgenic [Alb-K b mice (8,13,17,25)] expression, Des T cells activated by hepatocytes never developed into CTL, a finding similarly observed for OT-I T cells activated intrahepatically by de novo-expressed loweraffinity ligands. Overall, a wide variety of outcomes have been reported after intrahepatic CD8 T-cell activation in mice expressing transgenic liver antigens, including ignorance (33), deletional tolerance (8,13,17,25), and partial or full effector differentiation (11,12,24,34).…”

Section: Discussionmentioning

confidence: 94%

“…We recently described two mechanisms involved in impairing effector responses after intrahepatic activation: nonapoptotic degradation of T cells in hepatocyte lysosomes within the first day of activation ["suicidal emperipolesis" (25)] and Bimdependent apoptosis of T cells surviving suicidal emperipolesis (17). Although donor OT-I cells initially retained in the liver were efficiently deleted in mice treated with high-dose rAAV.…”

Section: Discussionmentioning

confidence: 99%

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Antigen expression level threshold tunes the fate of CD8 T cells during primary hepatic immune responses

Tay

Wong

McDonald

et al. 2014

Proc. Natl. Acad. Sci. U.S.A.

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115

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CD8 T-cell responses to liver-expressed antigens range from deletional tolerance to full effector differentiation resulting in overt hepatotoxicity. The reasons for these heterogeneous outcomes are not well understood. To identify factors that govern the fate of CD8 T cells activated by hepatocyte-expressed antigen, we exploited recombinant adenoassociated viral vectors that enabled us to vary potential parameters determining these outcomes in vivo. Our findings reveal a threshold of antigen expression within the liver as the dominant factor determining T-cell fate, irrespective of T-cell receptor affinity or antigen cross-presentation. Thus, when a low percentage of hepatocytes expressed cognate antigen, high-affinity T cells developed and maintained effector function, whereas, at a high percentage, they became functionally exhausted and silenced. Exhaustion was not irreversibly determined by initial activation, but was maintained by high intrahepatic antigen load during the early phase of the response; cytolytic function was restored when T cells primed under high antigen load conditions were transferred into an environment of low-level antigen expression. Our study reveals a hierarchy of factors dictating the fate of CD8 T cells during hepatic immune responses, and provides an explanation for the different immune outcomes observed in a variety of immune-mediated liver pathologic conditions. rAAV | CTL | TCR | cytotoxicity T he liver is acknowledged to possess unique tolerogenic properties, which have likely evolved to maintain immunological unresponsiveness toward food-derived and microbial antigens that enter the circulation via the gut (1, 2). This tolerogenic capability of the liver is demonstrated in animal models of liver transplantation, in which liver allografts are accepted across complete MHC mismatch barriers and are able to protect other donor tissues from rejection (reviewed in ref.3). In humans, the tolerogenic hepatic environment is likely to contribute to impaired immune clearance of the hepatitis B virus (HBV) and hepatitis C virus (HCV), which result in persistent infection in a significant proportion of exposed individuals and are associated with major morbidity and mortality. In contrast, effective immune responses to hepatotropic pathogens leading to resolution of infection are observed in most hepatitis A and E virus infections, the majority of individuals infected with HBV during adulthood, and a minority of those infected by HCV (reviewed in refs. 4, 5). The liver is also susceptible to a variety of autoimmune-mediated conditions (6). Collectively, these observations indicate that effective immune responses can be initiated and/or sustained in the liver despite its apparent predisposition toward the generation of tolerance. Unfortunately, there is no small animal model in which to study the parameters that determine the balance between intrahepatic immunity and tolerance in viral hepatitis. Thus, the factors that shape immune outcome have not yet been identified.By studying the fate of ...

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Section: Discussionsupporting

confidence: 67%

Section: Discussionmentioning

confidence: 94%

Section: Discussionmentioning

confidence: 99%

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Antigen expression level threshold tunes the fate of CD8 T cells during primary hepatic immune responses

Tay

Wong

McDonald

et al. 2014

Proc. Natl. Acad. Sci. U.S.A.

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115

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“…В случае пря-мого распознавания аллоантигенов на клетках эн-дотелия донорского органа (комплекса молекулы HLA I класса с аллоантигеным пептидом) наив-ными Т-лимфоцитами реципиента, имеющимися в циркуляции, происходит анергия и затем гибель апоптозом этих наивных Т-лимфоцитов из-за недо-статка ко-стимулирующих молекул [30,31]. Поэто-му при грамотно проведенной иммуносупрессии в организме не сохраняется стереотип клеток высо-коаффинной иммунологической памяти и после ре-генерации органа, а также элиминации АПК донора (вероятность острого отторжения как раз характе-ризует срок их жизни), процесс распознавания до-норских антигенов и формирование иммунного сте-реотипа начинается как бы заново.…”

Section: иммунобиологические закономерности формирования стереотипов unclassified

Individual Stability of Stereotypes of Immune Reacting and Modern Possibilities of Their Diagnostic in Organ Transplantation (Immune-Physiological Analysis of a Problem)

Onischenko¹,

Artamonov²,

Крашенинников³

et al. 2014

Russian Journal of Transplantology and Artificial Organs

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Лаборатория биотехнологии стволовых клеток (зав. -проф. Н.А. Онищенко) ФГБУ «ФНЦ трансплантологии и искусственных органов им. академика В.И. Шумакова» Министерства здравоохранения РФ (директор -академик РАМН, проф. С.В. Готье), Москва, Российская Федерация Авторы обосновывают варианты иммунного реагирования организма при трансплантации органов сущес-твованием индивидуальных специфических программ реагирования на аллоантигены, которые, исполь-зуя естественные активационные и тормозные механизмы, формируют различную степень устойчивости двух физиологических стереотипов «поведения иммунной системы» -эффекторного и толерогенного. Для идентификации индивидуального доминирующего стереотипа иммунного реагирования реципиента на трансплантат и прогнозирования изменений иммунного гомеостаза в организме авторы предлагают использовать показатели реактивности иммунной системы -консервативность и пластичность, которые могут быть выявлены подбором соответствующих биомаркеров. В настоящее время широко использует-ся система маркеров, характеризующих воспалительные реакции (инфекции/воспаления), для выявле-ния отторжения и сопутствующих осложнений. Для прогнозирования индивидуального доминирующего стереотипа реагирования при иммунологически спокойном течении посттрансплантационного периода авторы предлагают изучать систему информационно значимых клеточных маркеров адаптивного имму-нитета и использовать их для формирования комплексных информативных иммуно-клеточных диагнос-тических модулей.Ключевые слова: стереотипы иммунного ответа, трансплантация органов, биомаркеры. The authors prove variants of immune reacting of an human organism in organ transplantation by existence of individual specifi c programs of reacting on alloantigens which, using natural activatory and inhibitory mechanisms, form various degree of stability of two physiological stereotypes of "behavior of immune system" -effectoric and tolerogenic. For identifi cation of an individual predominant stereotype of recipient immune reacting on a graft and for forecasting changes of an immunological homeostasis in a human organism, authors suggest to use indexes of reactance of immune system -conservatism and plasticity which can be taped by selection of the conforming biomarkers. Now the system of markers characterizing infl ammatory reactions (infections/ infl ammation) for recognition organ rejection and related complications, is widely used. For forecasting of an individual dominant stereotype of reacting in immunologically quiet post-transplant follow-up authors suggest to study a system of informative cellular markers of adaptive immunity and to use them for a formation of complex informative diagnostic immuno-cellular modules. INDIVIDUAL STABILITY OF STEREOTYPES OF IMMUNE REACTING AND MODERN POSSIBILITIES OF THEIR DIAGNOSTIC IN ORGAN TRANSPLANTATION (IMMUNE-PHYSIOLOGICAL ANALYSIS OF A PROBLEM)

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“…We want to emphasize that to get to the discovery of new tumor biomarkers and/or molecular targets for new anticancer approaches, the mainstream approach is a genomic investigation, which in fact is not leading to remarkable and useful discovery for epochal changes in cancer patients' management. In fact, tumor cannibalism is included in a list of so called ''cell-in-cell phenomena'', together with entosis (overholtzer), ''emperitosis'', ''emperipolesis'' and ''suicidal emperipolesis'' [30][31][32][33][34] . An interesting debate on this issue may be read online in ''It's a Cell-Eat-Cell World'' By Jef Akst (1 August 2011, The Scientist).…”

Section: Example 2: Cancer Cells Behave As Amoebasmentioning

confidence: 99%

A nonmainstream approach against cancer

Fais

2016

Journal of Enzyme Inhibition and Medicinal Chemistry

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The discovery of antibiotics as specific and effective drugs against infectious agents has generated the belief that the famous Paul Erlich theory on magic bullet should be applied to cancer as well. However, after around 60 years of failures in finding a magic bullet against cancer, a question appears mandatory: does the magic bullet against cancer really exist? In trying to understand more on the issue, we propose three discoveries are coming from a nonmainstream approach against cancer. Tumor is acidic, and tumor acidity impairs drugs entering within tumor cells and isolates tumors from the rest of the body. Proton pumps are key in allowing tumor cells to live in the acidic microenvironment. A class of antiacidic drugs, proton pump inhibitors (PPIs), were shown to have a potent anti-tumor effect, through inhibition of proton pumps in tumor cells. PPIs are indeed prodrugs needing acidity to be activated into the active molecule. So they use protonation by H+ as an activating mechanism, while the vast majority of drugs are totally neutralized by protonation. An anti-tumor therapy based on PPI showed to be effective both in vitro and in vivo. Differently from normal cells, cancer cells meet their energy needs in great part by fermentation, and it appears conceivable that hypoxia and low nutrient transform tumor cells into fermenting anaerobes. This suggests that cancer cells are more similar to unicellular organisms, aimed at surviving in a continuous fighting, rather than cooperating, with other cells, as it occurs in the normal homeostasis of our body. We have shown that cancer cells take their fuel by ''cannibalizing'' other cells, either dead or alive, especially when starved and in acidic condition. This finding led to the discovery of a new oncogene TM9SF4 that human malignant cell shares with amoebas. The evidence is accumulating that almost all the cells release extracellular vehicles (EVs), from micro-to nanosize, which shuttle a variety of molecules. Tumor cells, particularly when stressed in their hostile microenvironment, release high levels of EVs, able to interact with target cells in various ways, within an organ or at a distance. They may represent both valuable tumor biomarker and shuttles for drugs with anti-tumor properties. This article wants to burst a real change in future anti-cancer strategies, based on the idea that tumors are much more common features than specific molecular targets.

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Hepatocyte entry leads to degradation of autoreactive CD8 T cells

Cited by 141 publications

References 32 publications

Antigen expression level threshold tunes the fate of CD8 T cells during primary hepatic immune responses

Antigen expression level threshold tunes the fate of CD8 T cells during primary hepatic immune responses

Individual Stability of Stereotypes of Immune Reacting and Modern Possibilities of Their Diagnostic in Organ Transplantation (Immune-Physiological Analysis of a Problem)

A nonmainstream approach against cancer

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