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Lichen sclerosus is associated with genital herpes simplex virus infection in a case-control study of 6,150 participants
Corresponding author: Dr. Shari R. Lipner, Department of Dermatology, Weill Cornell Medicine, New York, United States. shl9032@med.cornell.edu
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Received: ,
Accepted: ,
How to cite this article: Curtis KL, Stubblefield O, Sobieski B, Lipner SR. Lichen sclerosus is associated with genital herpes simplex virus infection in a case-control study of 6,150 participants. Indian J Dermatol Venereol Leprol. doi: 10.25259/IJDVL_1060_2024
Dear Editor,
Lichen sclerosus is a chronic inflammatory mucocutaneous disorder characterised by white atrophic plaques with erosions, painful ulcers, and permanent scar tissue, primarily affecting the anogenital region. Infectious organisms, including Borrelia burgdorferi, human papillomavirus, and hepatitis C virus, have been proposed as potential causes; however, evidence is conflicting and limited to small studies and case reports.1 Therefore, we aimed to assess lichen sclerosus associations with preceding infectious diagnoses using a large national database.
A nested case-control study using the National Institutes of Health All of Us database was conducted, with participants ≥18 years with lichen sclerosus diagnosis matched with controls 1:4 by age, sex at birth, and self-reported race/ethnicity. The All of Us programme is a national database dedicated to the enrollment of a diverse cohort of patients in the United States.2 We calculated multivariate logistic odds ratios for lichen sclerosus and preceding infectious diagnoses with matching by age, sex, and race/ethnicity. Infectious associations were diagnosed prior to lichen sclerosus diagnosis.
The analysis included 1,230 lichen sclerosus participants and 4,920 controls [Table 1]. Mean age of lichen sclerosus participants and controls was 68.5 years (P = 0.99). Among lichen sclerosus participants, 1109 participants (90.2%) were female and 941 participants (76.5%) were white, similar to controls (P = 1). Lichen sclerosus participants had higher odds of genital herpes simplex virus infection (OR = 3.79; 95% CI 2.64–5.45; P < 0.001) than controls [Table 2]. This difference persisted after stratifying the matched cohort by female lichen sclerosus participants (OR = 3.50; 95% CI 2.40–5.10; P < 0.001) and male lichen sclerosus participants (OR = 14.45; 95% CI 1.32–157.89; P = 0.02). Lichen sclerosus was not associated with chlamydia, Epstein Barr virus, gonorrhoea, hepatitis C, human immunodeficiency virus, human papillomavirus, Lyme, molluscum contagiosum, or syphilis.
| Controls (n = 4920) | Lichen sclerosus (n = 1230) | P value | |
|---|---|---|---|
| Age, mean (SD) | 68.5 (12.4) | 68.5 (12.4) | 0.99 |
| Sex at birth (%) | |||
| Male | 348 (7.1%) | 87 (7.1%) | 1 |
| Female | 4436 (90.2%) | 1109 (90.2%) | |
| Other | 136 (2.8%) | 34 (2.8%) | |
| Self-reported race/ethnicity count (%) | |||
| White | 3764 (76.5%) | 941 (76.5%) | 1 |
| Hispanic or Latino | 460 (9.4%) | 115 (9.4%) | |
| African American | 344 (7.0%) | 86 (7.0%) | |
| Asian or Other* | 352 (7.2%) | 88 (7.2%) |
| Associations (n, %) | Controls (n = 4920) | Lichen sclerosus (n = 1230) | OR (95% CI) | P value |
|---|---|---|---|---|
| Genital herpes simplex virus | 66 (1.3%) | 59 (4.8%) | 3.79 (2.64–5.45) | < 0.001 |
| Chlamydia | ≤20* | ≤20* | 1.76 (0.54–5.67) | 0.34 |
| Epstein Barr virus | ≤20* | ≤20* | 3.58 (0.48–26.35) | 0.21 |
| Gonorrhoea | ≤20* | ≤20* | 0.58 (0.10–3.2) | 0.54 |
| Hepatitis C | 117 (2.4%) | ≤20* | 0.67 (0.40–1.1) | 0.12 |
| Human immunodeficiency virus | 49 (1.0%) | ≤20* | 0.52 (0.22–1.21) | 0.13 |
| Human papilloma virus | 91 (1.8%) | 31 (2.5%) | 1.21 (0.79–1.86) | 0.36 |
| Lyme | 72 (1.5%) | ≤20* | 1.04 (0.62–1.73) | 0.86 |
| Molluscum contagiosum | ≤20* | ≤20* | 0.71 (0.08–6.26) | 0.76 |
| Syphilis | 22 (0.4%) | ≤20* | 0.88 (0.32–2.40) | 0.81 |
Infectious diagnoses preceded lichen sclerosus diagnosis. Statistical analyses were conducted using R (version 4.40).
Goodness-of-fit test: Chi-squared = .1304, degrees of freedom (df) = 0, p = 0.
Boldface indicates significance (P < 0.05).
OR: Odds ratio, CI: Confidence interval.
To our knowledge, this is the first case-control study to assess for multiple potential lichen sclerosus infectious associations. Lichen sclerosus participants had an almost four-fold risk of prior genital herpes simplex virus diagnosis, which is a striking finding. This association may be potentially related to chronic trauma from recurrent genital herpes episodes, similar to other lichen sclerosus associations related to irritation and trauma, including urinary incontinence, multiparous status, and high body mass index. Additionally, occlusion, scratching, friction, surgical procedures, and injections may act as a Koebner phenomenon leading to lichen sclerosus development. Alternatively, our finding may be related to the initial misdiagnosis of lichen sclerosus as genital herpes due to overlapping clinical features, including erosions, painful ulcers, dysuria, dyspareunia, and pruritus.
Concomitant genital herpes simplex virus infection and lichen sclerosus have been rarely reported in the literature and poses a therapeutic challenge, since topical corticosteroids may reactivate genital herpes and delay herpes simplex virus lesion healing.3 In one case report of a lichen sclerosus patient with genital herpes simplex virus infection, treatment with systemic acyclovir 400 mg three times daily for seven days and topical clobetasol propionate 0.05% cream for ten days, followed by acyclovir 400 mg twice daily and clobetasol propionate 0.05% cream for one month resulted in lesion resolution after 30 days.3
We did not find lichen sclerosus association with human papillomavirus. The role of human papillomavirus in lichen sclerosus pathogenesis is controversial, with one study of 88 male lichen sclerosus cases reporting the presence of human papillomavirus deoxyribonucleic acid in biopsy specimens of 37.5% of cases, most commonly human papillomavirus type 16.4 In another case series of 329 patients, there was no correlation between male genital lichen sclerosus and human papillomavirus.5
We did not find lichen sclerosus association with Lyme disease. In a prospective study6 of 61 lichen sclerosus cases and 118 controls, Borrelia species was detected in 63% of lichen sclerosus specimens and was absent in all negative controls. In contrast, borrelial deoxyribonucleic acid was not detected in any serological studies or skin biopsy specimens in a prospective study7 of eight lichen sclerosus patients.
We did not find lichen sclerosus association with hepatitis C. A lipidomic and metabolomic analysis demonstrated that vulvar lichen sclerosus correlated with an abnormal antiviral response due to the presence of hepatitis C virus poly-U/UC sequences.8 In contrast, in a prospective study9 of 61 male patients with genital lichen sclerosus, no patients had hepatitis C virus seropositivity.
Limitations include lack of histopathologic confirmation of lichen sclerosus and herpes simplex virus confirmation via viral culture, potential disease misclassification, inability to measure time between herpes simplex virus infection and lichen sclerosus diagnosis, exclusion of pediatric participants in the database, and small male sample size. Strengths include an overall large sample size and a case-control design.
In conclusion, we demonstrate a novel finding of lichen sclerosus association with genital herpes simplex virus infection. Our data argues against previously hypothesised infectious associations with human papillomavirus, Lyme disease, and hepatitis C. Studies utilising histopathology and viral culture for diagnostic confirmation are needed to corroborate these findings. We recommend that dermatologists elicit history of genital herpes simplex virus infection and perform a complete examination of the anogenital area for herpes simplex virus infection and lichen sclerosus. Consideration of antiviral suppressive therapy in patients with recurrent herpes simplex virus infection might prevent worsening of lichen sclerosus.
Ethical approval
This study was approved by the Institutional Review Board of Weill Cornell Medicine (record #: 19-11021049).
Declaration of patient consent
The authors certify that they have obtained all appropriate patient consent.
Financial support and sponsorship
The All of Us Research Program is supported by the National Institutes of Health, Office of the Director: Regional Medical Centers: 1 OT2 OD026549; 1 OT2 OD026554; 1 OT2 OD026557; 1 OT2 OD026556; 1 OT2 OD026550; 1 OT2 OD 026552; 1 OT2 OD026553; 1 OT2 OD026548; 1 OT2 OD026551; 1 OT2 OD026555; IAA #: AOD 16037; Federally Qualified Health Centers: HHSN 263201600085U; Data and Research Center: 5 U2C OD023196; Biobank: 1 U24 OD023121; The Participant Center: U24 OD023176; Participant Technology Systems Center: 1 U24 OD023163; Communications and Engagement: 3 OT2 OD023205; 3 OT2 OD023206; and Community Partners: 1 OT2 OD025277; 3 OT2 OD025315; 1 OT2 OD025337; 1 OT2 OD025276.
Conflicts of interest
There are no conflicts of interest.
Use of artificial intelligence (AI)-assisted technology for manuscript preparation
The authors confirm that there was no use of AI-assisted technology for assisting in the writing or editing of the manuscript and no images were manipulated using AI.
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