Journal of Peking University (Health Sciences) ›› 2022, Vol. 54 ›› Issue (2): 267-271. doi: 10.19723/j.issn.1671-167X.2022.02.011

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Consistency analysis and clinical guiding significance of cytomegalovirus nucleic acid and antibody detections in patients with different clinical characteristics

DAI Ju-hua1,SUN Xin-ping1,ZHANG Jie1,SHI Lian-jie2,()   

  1. 1. Department of Clinical Laboratory, Peking University International Hospital, Beijing 102206, China
    2. Department of Rheumatology and Immunology, Peking University International Hospital, Beijing 102206, China
  • Received:2020-04-06 Online:2022-04-18 Published:2022-04-13
  • Contact: Lian-jie SHI E-mail:shilianjie@pkuih.edu.cn
  • Supported by:
    National Natural Science Foundation of China(81501396);Peking University International Hospital Research Funds(YN2017QX01)

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Abstract:

Objective: To investigate the consistency of cytomegalovirus deoxyribo nucleic acid (CMV-DNA) and immunoglobulin M (IgM) antibody detections in patients with different clinical characteristics and their guiding value for clinical practice. Methods: From December 2014 to November 2019, a total of 507 patients who were detected with both CMV-IgM and CMV-DNA were collected in Peking University International Hospital. Their general information, such as gender, age and clinical data, including the patient’s diagnosis, medication, and outcome were also collected. The groups were stratified according to whether CMV-DNA was negative or positive, CMV-IgM was negative or positive, age, gender, and whether they received immunosuppressive therapy or not. The Pearson Chi-square test or Fisher’s exact test was used for comparison of the rates between the groups. P<0.05 means the difference is statisti-cally significant. Results: Of the 507 patients submitted for examination, 55 (10.85%) were positive for CMV-DNA, 74 (14.60%) were positive for CMV-IgM, and 20 (3.94%) were positive for both CMV-DNA and CMV-IgM. Of the 55 patients with CMV-DNA positive, 37 were male, accounting for 67.27%. In addition, 25 patients were older than 60 years, accounting for 45.45% and 33 patients received immunosuppressive therapy, accounting for 60%. The rates were higher than that of CMV-DNA negative group, 47.35% (P=0.005), 68.14% (P=0.043), 46.02% (P=0.050), respectively. Of the patients with both CMV-DNA and IgM positive, 45% received immunosuppressive threapy, which was lower than that of CMV-DNA positive but IgM negative patients (68.57%, P=0.086), and also lower than CMV-DNA negative but IgM positive patients (68.52%, P=0.064). In the patients with both CMV-DNA and IgM positive, 91.67% showed remission after receiving ganciclovir, whereas in the patients with CMV-DNA positive but IgM negative, the rate was only 60% (P=0.067). Conclusion: CMV-IgM antibody detection is affected by age, gender, and immune status. It is not recommended to use CMV-IgM alone to determine CMV infection in patients with immunosuppressive status and those older than 60 years. CMV-DNA and CMV-IgM combined detection may help to predict patients’ immune status and outcomes of antiviral therapy.

Key words: Cytomegalovirus, DNA, Immunoglobulin M, Immunosuppression

CLC Number: 

  • R446

Table 1

Comparison of the results of CMV-IgM and CMV-DNA tests"

Items CMV-DNA (+) CMV-DNA (-) Total
CMV-IgM (+) 20 54 74
CMV-IgM (-) 35 398 433
Total 55 452 507

Table 2

Overview of characteristics of 507 patients suspected CMV infection"

Items CMV-DNA (+),
n (%)
CMV-DNA (-),
n (%)
P
Gender 0.005
Male 37 (67.27) 214 (47.35)
Female 18 (32.73) 238 (52.65)
Age 0.043
<60 years 30 (54.55) 308 (68.14)
≥60 years 25 (45.45) 144 (31.86)
Immunosuppressant 0.050
Yes 33 (60.00) 208 (46.02)
No 22 (40.00) 244 (53.98)

Table 3

Comparison of the consistency of CMV-DNA and CMV-IgM detection in patients with different characteristics"

Items CMV-DNA (+), n (%) CMV-IgM (+), n (%)
CMV-IgM (+) CMV-IgM (-) P CMV-DNA (+) CMV-DNA (-) P
Gender 0.356 0.054
Male 15 (75.00) 22 (62.86) 15 (75.00) 27 (50.00)
Female 5 (25.00) 13 (37.14) 5 (25.00) 27 (50.00)
Age 0.799 0.153
<60 years 11 (55.00) 18 (51.43) 11 (55.00) 40 (74.07)
≥60 years 9 (45.00) 17 (48.57) 9 (45.00) 14 (25.93)
Immunosuppressant 0.086 0.064
Yes 9 (45.00) 24 (68.57) 9 (45.00) 37 (68.52)
No 11 (55.00) 11 (31.43) 11 (55.00) 17 (31.48)

Table 4

Analysis of the response of patients with CMV infection with different characteristics to anti-CMV therapy (ganciclovir)"

Response CMV-DNA (+), n (%) CMV-DNA (+), n (%)
With immunosuppressant Without immunosuppressant P CMV-IgM (+) CMV-IgM (-) P
Remission 19 (65.52) 10 (76.92) 0.719 11 (91.67) 18 (60.00) 0.067
Poor 10 (34.48) 3 (23.08) 1 (8.33) 12 (40.00)
[1] 阮强. 人巨细胞病毒感染的实验室检测与诊断[J]. 实用儿科临床杂志, 2012, 27(10):729-731.
[2] 陈兰兰, 倪安平. 免疫抑制患者巨细胞病毒感染的实验室检测及临床意义[J]. 中华检验医学杂志, 2014, 37(2):155-158.
[3] 王晗, 李廷栋, 郭小怡. 巨细胞病毒实验室检测方法研究进展及其用于新生儿筛查的可行性[J]. 临床儿科杂志, 2018, 36(3):221-226.
[4] 李玲霞, 高申, 张特, 等. 人巨细胞病毒感染DNA检测和IgM检测的比较及其联合应用价值的探讨[J]. 中国实验诊断学, 2015(1):78-80.
[5] 陈雁汶. 血清学检测和聚合酶链反应在急性和慢性巨细胞病毒感染监测中的比较[J]. 检验医学, 2016, 31(6):458-461.
[6] Furui Y, Satake M, Hoshi Y, et al. Cytomegalovirus (CMV) seroprevalence in Japanese blood donors and high detection frequency of CMV DNA in elderly donors[J]. Transfusion, 2013, 53(10):2190-2197.
[7] Yoshida M, Matsuda H, Yoshinaga Y, et al. Can measurement of maternal anti-cytomegalovirus immunoglobulin-M antibody levels be used to screen for cytomegalovirus infection in embryos and fetuses?[J]. J Obstet Gynaecol Res, 2013, 39(1):166-169.
doi: 10.1111/j.1447-0756.2012.01900.x
[8] 李婧辰, 张梅, 李镒冲, 等. 我国40岁及以上人群慢性呼吸系统疾病症状流行现况及影响因素研究[J]. 中华流行病学杂志, 2018, 39(6):786-791.
[9] Mirza S, Clay RD, Koslow MA, et al. Copd guidelines: A review of the 2018 gold report[J]. Mayo Clin Proc, 2018, 93(10):1488-1502.
doi: 10.1016/j.mayocp.2018.05.026
[10] Fava A, Petri M. Systemic lupus erythematosus: Diagnosis and clinical management[J]. J Autoimmun, 2019, 96:1-13.
doi: 10.1016/j.jaut.2018.11.001
[11] Lisnevskaia L, Murphy G, Isenberg D. Systemic lupus erythematosus[J]. Lancet, 2014, 384(9957):1878-1888.
doi: S0140-6736(14)60128-8 pmid: 24881804
[12] 邓晓莉, 迟妮妮, 李欣艺, 等. 系统性红斑狼疮患者巨细胞病毒感染的临床特点分析[J]. 中华风湿病学杂志, 2016, 20(6):378-381.
[13] Rasmussen NS, Draborg AH, Nielsen CT, et al. Antibodies to early EBV, CMV, and HHV6 antigens in systemic lupus erythematosus patients[J]. Scand J Rheumatol, 2015, 44(2):143-149.
doi: 10.3109/03009742.2014.973061 pmid: 25562120
[14] Perez-Mercado AE, Vila-Perez S. Cytomegalovirus as a trigger for systemic lupus erythematosus[J]. J Clin Rheumatol, 2010, 16(7):335-337.
doi: 10.1097/RHU.0b013e3181f4cf52
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