PD-1 Signaling Has a Critical Role in Maintaining Regulatory T Cell Homeostasis; Implication for Treg Depletion Therapy By PD-1 Blockade

Asano, Takeru; Kishi, Yoshiki; Meguri, Yusuke; Yoshioka, Tomoko; Iwamoto, Miki; Maeda, Yoshinobu; Yagita, Hideo; Tanimoto, Mitsune; Koreth, John; Ritz, Jérôme; Matsuoka, Ken‐ichi

doi:10.1182/blood.v126.23.848.848

Cited by 14 publications

(10 citation statements)

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“…Furthermore, PD-1 may suppress the proliferation of T regulatory cells (Tregs). The blockade of PD-1 may promote the proliferation of Tregs that leads to increased immunosuppression, hence the reactivation of HBV [23, 24]. In line with these inconsistent hypotheses, the only clinical trial with anti-PD-1 antibody for non-cancer patients with viral hepatitis showed that even though some patients have persistent suppression of HCV replication, only 5 of 42 patients (12%) met the primary endpoint of a ≥ 0.5 log reduction in HCV RNA [25].…”

Section: Discussionmentioning

confidence: 99%

Hepatitis B virus reactivation in cancer patients with positive Hepatitis B surface antigen undergoing PD-1 inhibition

Zhang¹,

Zhou²,

Chen³

et al. 2019

j. immunotherapy cancer

135

142

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BackgroundHepatitis B virus (HBV) reactivation is a serious complication in patients with cancers and HBV infection undergoing immunosuppressant treatment or chemotherapy. However, the safety of anti-programmed cell death (PD) -1 and anti-programmed cell death-ligand 1 (PD-L1) therapy in these patients is unknown because they were excluded from clinical trials of immunotherapy.MethodsThis retrospective cohort study involved consecutive hepatitis B surface antigen (HBsAg) -positive cancer patients who were referred to Sun Yat-sen University Cancer Center and received an anti-PD-1/PD-L1 antibody between January 1, 2015 and July 31, 2018. The primary end point was the rate of the occurrence of HBV reactivation.ResultsIn total, 114 eligible patients were included, among whom 90 (79%) were male, and the median (range) age was 46 (16–76) years. Six patients (5.3%) developed HBV reactivation, occurring at a median of 18 weeks (range, 3–35 weeks) from the commencement of immunotherapy. Among these patients, all of them had undetectable baseline HBV DNA; one had prophylactic antiviral therapy while five did not; four were positive for Hepatitis B e antigen while the other two were negative. At reactivation, the median HBV DNA level was 3.89 × 104 IU/mL (range, 1.80 × 103–6.00 × 107 IU/mL); five had HBV-related hepatitis and one exhibited increasing HBV DNA level without alanine transaminase elevation. No HBV-related fatal events occurred. The lack of antiviral prophylaxis was the only significant risk factor for HBV reactivation (odds ratio, 17.50 [95% CI, 1.95–157.07], P = .004).ConclusionsHBV reactivation occurs in a subset of HBsAg-positive cancer patients undergoing anti-PD-1 or anti-PD-L1 immunotherapy. Regular monitoring of HBV DNA and antiviral prophylaxis are advised to prevent this potentially fatal complication.

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Section: Discussionmentioning

confidence: 99%

Hepatitis B virus reactivation in cancer patients with positive Hepatitis B surface antigen undergoing PD-1 inhibition

Zhang¹,

Zhou²,

Chen³

et al. 2019

j. immunotherapy cancer

135

142

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“…CTLA4 + Tregs increase during HIV infection [ 9 , 16 , 17 ] and remains higher despite antiretroviral therapy (ART) [18] . PD1 is expressed on Tregs under resting and activated conditions [ 19 , 20 ] and prevents the proliferation and immune responses of effector T-cells [ 21 , 22 ]. Untreated HIV infection increases PD1 + Tregs, and their levels positively correlate with viral load and exhaustion of total CD4 and CD8 T-cells [23] .…”

Section: Introductionmentioning

confidence: 99%

Dynamics and epigenetic signature of regulatory T-cells following antiretroviral therapy initiation in acute HIV infection

et al. 2021

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Background: HIV infection promotes the expansion of immunosuppressive regulatory T-cells (Tregs), contributing to immune dysfunction, tissue fibrosis and disease progression. Early antiretroviral treatment (ART) upon HIV infection improves CD4 count and decreases immune activation. However, Treg dynamics and their epigenetic regulation following early ART initiation remain understudied. Methods: Treg subsets were characterized by flow cytometry in 103 individuals, including untreated HIVinfected participants in acute and chronic phases, ART-treated in early infection, elite controllers (ECs), immunological controllers (ICs), and HIV-uninfected controls. The methylation status of six regulatory regions of the foxp3 gene was assessed using MiSeq technology. Findings: Total Treg frequency increased overtime during HIV infection, which was normalized in early ART recipients. Tregs in untreated individuals expressed higher levels of activation and immunosuppressive markers (CD39, and LAP(TGF-b1)), which remained unchanged following early ART. Expression of gut migration markers (CCR9, Integrin-b7) by Tregs was elevated during untreated HIV infection, while they declined with the duration of ART but not upon early ART initiation. Notably, gut-homing Tregs expressing LAP(TGF-b1) and CD39 remained higher despite early treatment. Additionally, the increase in LAP(TGF-b1) + Tregs overtime were consistent with higher demethylation of conserved non-coding sequence (CNS)-1 in the foxp3 gene. Remarkably, LAP(TGF-b1)-expressing Tregs in ECs were significantly higher than in uninfected subjects, while the markers of Treg activation and gut migration were not different. Interpretation: Early ART initiation was unable to control the levels of immunosuppressive Treg subsets and their gut migration potential, which could ultimately contribute to gut tissue fibrosis and HIV disease progression. Funding: This study was funded by the Canadian Institutes of Health Research (CIHR, grant MOP 142294) and in part by the AIDS and Infectious Diseases Network of the R eseau SIDA et maladies infectieuses du Fonds de recherche du Qu ebec-Sant e (FRQ-S).

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“…As mentioned earlier, Tregs also express PD-1, which affected their homeostasis ( 17 , 220 ). PD-1 also is thought to participate in Treg suppression ( 221 ).…”

Section: Therapies Targeting Treg Functionmentioning

confidence: 79%

Regulatory T Cells As Potential Targets for HIV Cure Research

et al. 2018

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T regulatory cells (Tregs) are a key component of the immune system, which maintain a delicate balance between overactive responses and immunosuppression. As such, Treg deficiencies are linked to autoimmune disorders and alter the immune control of pathogens. In HIV infection, Tregs play major roles, both beneficial and detrimental. They regulate the immune system such that inflammation and spread of virus through activated T cells is suppressed. However, suppression of immune activation also limits viral clearance and promotes reservoir formation. Tregs can be directly targeted by HIV, thereby harboring a fraction of the viral reservoir. The vital role of Tregs in the pathogenesis and control of HIV makes them a subject of interest for manipulation in the search of an HIV cure. Here, we discuss the origin and generation, homeostasis, and functions of Tregs, particularly their roles and effects in HIV infection. We also present various Treg manipulation strategies, including Treg depletion techniques and interventions that alter Treg function, which may be used in different cure strategies, to simultaneously boost HIV-specific immune responses and induce reactivation of the latent virus.

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PD-1 Signaling Has a Critical Role in Maintaining Regulatory T Cell Homeostasis; Implication for Treg Depletion Therapy By PD-1 Blockade

Cited by 14 publications

References 0 publications

Hepatitis B virus reactivation in cancer patients with positive Hepatitis B surface antigen undergoing PD-1 inhibition

Hepatitis B virus reactivation in cancer patients with positive Hepatitis B surface antigen undergoing PD-1 inhibition

Dynamics and epigenetic signature of regulatory T-cells following antiretroviral therapy initiation in acute HIV infection

Regulatory T Cells As Potential Targets for HIV Cure Research

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