Impact of induction agents and maintenance immunosuppression on torque teno virus loads and year-one complications after kidney transplantation.

IF 5.7 2区医学 Q1 IMMUNOLOGY Frontiers in Immunology Pub Date : 2024-11-13 eCollection Date: 2024-01-01 DOI:10.3389/fimmu.2024.1492611

Marvin Reineke, Claudius Speer, Christian Bundschuh, Julian A F Klein, Lisa Loi, Claudia Sommerer, Martin Zeier, Paul Schnitzler, Christian Morath, Louise Benning

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Abstract

Background: Torque teno virus load (TTVL) is gaining importance as a surrogate parameter to assess immunocompetence in kidney transplant recipients. Although the dynamics of TTVL have been investigated before, the impact of different induction agents and variations in immunosuppressive maintenance therapies on TTVL remain unknown.

Methods: In this retrospective study, TTVL was quantified in 537 plasma or serum samples from 134 patients transplanted between 2018 and 2021. TTVL was examined pre-transplantation and 30-, 90-, 180-, and 360-days post-transplant. To assess the influence of induction therapy on TTVL, 67 patients receiving anti-thymocyte globulin (ATG) induction were matched with 67 patients receiving an interleukin-2 receptor antagonist (IL2-RA) induction in terms of age, sex, and donor modality.

Results: Following transplantation, there was a steep increase in TTVL post-transplant for all patients with peak viral loads at 90 days post-transplant (median TTVL [IQR] 7.97×10⁶, [4.50×10⁵-1.12×10⁸]) followed by subsequently declining viral loads. Compared to patients receiving IL2-RA as induction therapy, patients receiving ATG had significantly higher peak viral loads 3 months post-transplant (median TTVL [IQR] 2.82×10⁷ [3.93×10⁶-1.30×10⁸] vs. median TTVL [IQR] 2.40×10⁶ [5.73×10⁴-2.60×10⁷]; P<0.001). Throughout all post-transplant time points, patients receiving additional rituximab for induction along with higher tacrolimus target levels exhibited the highest TTVL.Patients whose TTVL 3-months post-transplant exceeded the currently proposed cutoff to predict infections within the first year post-transplant [6.2 log₁₀] showed a trend towards a higher risk of being hospitalized with an infection in the following 9 months, albeit without being statistically significant (HR=1.642, P=0.07).

Conclusions: Higher TTVL reflects the greater immunosuppressive burden in immunological high-risk patients receiving intensive immunosuppression. The choice of induction agent and intensified immunosuppressive maintenance therapy notably affects TTVL at 3 months post-transplant and beyond, necessitating careful consideration when interpreting and applying TTVL cutoffs to monitor immunocompetence post-transplant.

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诱导剂和维持性免疫抑制剂对肾移植术后转矩特诺病毒载量和第一年并发症的影响。

背景：作为评估肾移植受者免疫能力的替代参数，Torque teno病毒载量（TTVL）正变得越来越重要。虽然以前曾对 TTVL 的动态进行过研究，但不同诱导剂和免疫抑制维持疗法的变化对 TTVL 的影响仍然未知：在这项回顾性研究中，对2018年至2021年间移植的134名患者的537份血浆或血清样本中的TTVL进行了量化。对移植前、移植后30天、90天、180天和360天的TTVL进行了检测。为了评估诱导治疗对TTVL的影响，67名接受抗胸腺细胞球蛋白（ATG）诱导的患者与67名接受白细胞介素-2受体拮抗剂（IL2-RA）诱导的患者在年龄、性别和供体方式方面进行了配对：移植后，所有患者的TTVL都急剧上升，病毒载量在移植后90天达到峰值（中位数TTVL [IQR] 7.97×106，[4.50×105-1.12×108]），随后病毒载量下降。与接受 IL2-RA 诱导治疗的患者相比，接受 ATG 的患者在移植后 3 个月的病毒载量峰值明显更高（中位数 TTVL [IQR] 2.82×107 [3.93×106-1.30×108] 与中位数 TTVL [IQR] 2.40×106[5.73×104-2.60×107]；P10]显示，在随后的9个月中，因感染住院的风险有升高的趋势，但无统计学意义（HR=1.642，P=0.07）：较高的TTVL反映了接受强化免疫抑制的免疫高危患者的免疫抑制负担较重。诱导药物和强化免疫抑制维持疗法的选择对移植后3个月及以后的TTVL有显著影响，因此在解释和应用TTVL临界值以监测移植后免疫能力时必须慎重考虑。

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来源期刊

Frontiers in Immunology IMMUNOLOGY-

CiteScore

9.80

自引率

11.00%

发文量

7153

审稿时长

14 weeks

期刊介绍： Frontiers in Immunology is a leading journal in its field, publishing rigorously peer-reviewed research across basic, translational and clinical immunology. This multidisciplinary open-access journal is at the forefront of disseminating and communicating scientific knowledge and impactful discoveries to researchers, academics, clinicians and the public worldwide. Frontiers in Immunology is the official Journal of the International Union of Immunological Societies (IUIS). Encompassing the entire field of Immunology, this journal welcomes papers that investigate basic mechanisms of immune system development and function, with a particular emphasis given to the description of the clinical and immunological phenotype of human immune disorders, and on the definition of their molecular basis.