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利用供体特异性抗体和移植物功能障碍重新定义心脏抗体介导的排斥反应。

Redefining Cardiac Antibody-Mediated Rejection With Donor-Specific Antibodies and Graft Dysfunction.

作者信息

Goldberg Jason F, Tian Xin, Bon Ann, Xu Yifei, Gerhard Eleanor, Brower Ruth, Jang Moon Kyoo, Kong Hyesik, Andargie Temesgen E, Park Woojin, Najjar Samer S, Tchoukina Inna, Shah Keyur B, Hsu Steven, Rodrigo Maria E, Marboe Charles, Berry Gerald J, Valantine Hannah A, Shah Palak, Agbor-Enoh Sean

机构信息

Inova Schar Heart and Vascular, Falls Church, VA (J.F.G., P.S.).

Inova L.J. Murphy Children's Hospital, Falls Church, VA (J.F.G.).

出版信息

Circ Heart Fail. 2024 Dec;17(12):e011592. doi: 10.1161/CIRCHEARTFAILURE.124.011592. Epub 2024 Nov 25.

Abstract

BACKGROUND

Heart transplant recipients with donor-specific antibodies (DSAs) have an increased risk for antibody-mediated rejection. However, many patients with graft dysfunction and DSA do not have evidence of antibody-mediated rejection by endomyocardial biopsy (EMB).

METHODS

Participants from this prospective, multicenter study underwent serial EMB, echocardiogram, DSA, and donor-derived cell-free DNA evaluations. Outcomes were defined as pAMR+ (pAMR≥1) or DSA+/left ventricle (LV) dysfunction (DSA presence+LVEF drop ≥10% to an LVEF≤50%). Cox regression evaluated the association between antibody-mediated rejection categories and death or sustained (for 3 months) reduction of LVEF to <50%.

RESULTS

Two hundred sixteen patients (29% women, 39% Black race, median age 55 [interquartile range, 47-62] years) had 1488 EMB, 2792 DSA, 1821 echocardiograms, and 1190 donor-derived cell-free DNA evaluations. DSAs were present in 86 patients (40%). Fourteen patients had isolated pAMR+ episodes and 8 patients had isolated DSA+/LV dysfunction episodes; 2 patients had pAMR+ and then subsequently DSA+/LV dysfunction with pAMR+. Median %dd-cfDNA was significantly higher at diagnosis of pAMR+ (0.63% [interquartile range, 0.23-2.0]; =0.0002), or DSA+/LV dysfunction (0.40% [interquartile range, 0.36-1.24]; <0.0001), compared with patients without these outcomes (0.01% [interquartile range, 0.0001-0.10]). Both pAMR+ and DSA+/LV dysfunction were associated with long-term clinical outcome of death (n=18) or prolonged LV dysfunction (n=10): pAMR+ (hazard ratio, 2.8 [95% CI, 1.03-7.4]; =0.043); DSA+/LV dysfunction (hazard ratio, 26.2 [95% CI, 9.6-71.3]; <0.001); composite of both definitions (hazard ratio, 6.5 [95% CI, 2.9-14.3]; <0.001). Patients who developed pAMR+ or DSA+/LV dysfunction within the first 6 months of transplant were more likely to die within 3 years posttransplant (hazard ratio, 3.9 [95% CI, 1.03-14.6]; =0.031).

CONCLUSIONS

Expanding the characterization of antibody-mediated rejection to include patients with DSA and concurrent allograft dysfunction identified DSA+ patients at risk for death and prolonged LV dysfunction.

摘要

背景

携带供体特异性抗体(DSA)的心脏移植受者发生抗体介导排斥反应的风险增加。然而,许多出现移植物功能障碍且携带DSA的患者经心内膜心肌活检(EMB)未发现抗体介导排斥反应的证据。

方法

这项前瞻性多中心研究的参与者接受了系列EMB、超声心动图、DSA及供体来源游离DNA评估。结局定义为pAMR+(pAMR≥1)或DSA+/左心室(LV)功能障碍(存在DSA+左心室射血分数[LVEF]下降≥10%至LVEF≤50%)。Cox回归评估抗体介导排斥反应类别与死亡或LVEF持续(3个月)降至<50%之间的关联。

结果

216例患者(29%为女性,39%为黑人,中位年龄55[四分位间距,47 - 62]岁)接受了1488次EMB、2792次DSA、1821次超声心动图及1190次供体来源游离DNA评估。86例患者(40%)存在DSA。14例患者出现孤立性pAMR+发作,8例患者出现孤立性DSA+/LV功能障碍发作;2例患者先出现pAMR+,随后出现伴有pAMR+的DSA+/LV功能障碍。与未出现这些结局的患者(0.01%[四分位间距,0.0001 - 0.10])相比,pAMR+(0.63%[四分位间距,0.23 - 2.0];P = 0.0002)或DSA+/LV功能障碍(0.40%[四分位间距,0.36 - 1.24];P < 0.0001)诊断时的中位%dd - cfDNA显著更高。pAMR+和DSA+/LV功能障碍均与死亡(n = 18)或长期LV功能障碍(n = 10)的长期临床结局相关:pAMR+(风险比,2.8[95%CI,1.03 - 7.4];P = 0.043);DSA+/LV功能障碍(风险比,26.2[95%CI,9.6 - 71.3];P < 0.001);两种定义的复合情况(风险比,6.5[95%CI,2.9 - 14.3];P < 0.001)。在移植后前6个月内出现pAMR+或DSA+/LV功能障碍的患者在移植后3年内死亡的可能性更大(风险比,3.9[95%CI,1.03 - 14.6];P = 0.031)。

结论

将抗体介导排斥反应的特征扩展至包括携带DSA及并发同种异体移植物功能障碍的患者,可识别出有死亡风险及长期LV功能障碍风险的DSA+患者。

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