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Endogenous intronic antisense long non-coding RNA, MGAT3-AS1, and kidney transplantation
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Abstractβ-1,4-mannosylglycoprotein 4-β-N-acetylglucosaminyltransferase (MGAT3) is a key molecule for the innate immune system. We tested the hypothesis that intronic antisense long non-coding RNA, MGAT3-AS1, can predict delayed allograft function after kidney transplantation. We prospectively assessed kidney function and MGAT3-AS1 in 129 incident deceased donor kidney transplant recipients before and after transplantation. MGAT3-AS1 levels were measured in mononuclear cells using qRT-PCR. Delayed graft function was defined by at least one dialysis session within 7 days of transplantation. Delayed graft function occurred in 22 out of 129 transplant recipients (17%). Median MGAT3-AS1 after transplantation was significantly lower in patients with delayed graft function compared to patients with immediate graft function (6.5 × 10−6, IQR 3.0 × 10−6 to 8.4 × 10−6; vs. 8.3 × 10−6, IQR 5.0 × 10−6 to 12.8 × 10−6; p < 0.05). The median preoperative MGAT3-AS1 was significantly lower in kidney recipients with delayed graft function (5.1 × 10−6, IQR, 2.4 × 10−6 to 6.8 × 10−6) compared to recipients with immediate graft function (8.9 × 10−6, IQR, 6.8 × 10−6 to 13.4 × 10−6; p < 0.05). Receiver-operator characteristics showed that preoperative MGAT3-AS1 predicted delayed graft function (area under curve, 0.83; 95% CI, 0.65 to 1.00; p < 0.01). We observed a positive predictive value of 0.57, and a negative predictive value of 0.95. Long non-coding RNA, MGAT3-AS1, indicates short-term outcome in patients with deceased donor kidney transplantation.
Springer Science and Business Media LLC
Title: Endogenous intronic antisense long non-coding RNA, MGAT3-AS1, and kidney transplantation
Description:
Abstractβ-1,4-mannosylglycoprotein 4-β-N-acetylglucosaminyltransferase (MGAT3) is a key molecule for the innate immune system.
We tested the hypothesis that intronic antisense long non-coding RNA, MGAT3-AS1, can predict delayed allograft function after kidney transplantation.
We prospectively assessed kidney function and MGAT3-AS1 in 129 incident deceased donor kidney transplant recipients before and after transplantation.
MGAT3-AS1 levels were measured in mononuclear cells using qRT-PCR.
Delayed graft function was defined by at least one dialysis session within 7 days of transplantation.
Delayed graft function occurred in 22 out of 129 transplant recipients (17%).
Median MGAT3-AS1 after transplantation was significantly lower in patients with delayed graft function compared to patients with immediate graft function (6.
5 × 10−6, IQR 3.
0 × 10−6 to 8.
4 × 10−6; vs.
8.
3 × 10−6, IQR 5.
0 × 10−6 to 12.
8 × 10−6; p < 0.
05).
The median preoperative MGAT3-AS1 was significantly lower in kidney recipients with delayed graft function (5.
1 × 10−6, IQR, 2.
4 × 10−6 to 6.
8 × 10−6) compared to recipients with immediate graft function (8.
9 × 10−6, IQR, 6.
8 × 10−6 to 13.
4 × 10−6; p < 0.
05).
Receiver-operator characteristics showed that preoperative MGAT3-AS1 predicted delayed graft function (area under curve, 0.
83; 95% CI, 0.
65 to 1.
00; p < 0.
01).
We observed a positive predictive value of 0.
57, and a negative predictive value of 0.
95.
Long non-coding RNA, MGAT3-AS1, indicates short-term outcome in patients with deceased donor kidney transplantation.
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