More than a skin disease: stress, depression, anxiety levels, and serum neurotrophins in lichen simplex chronicus<sup>,</sup>

Altunay, İlknur Kivanç; Özkur, Ezgi; Ugurer, Ece; Baltan, Ecem; Aydin, Çigdem; Serin, Erdinç

doi:10.1016/j.abd.2021.04.011

Abstract

Background:

Lichen simplex chronicus is a dermatological condition due to excessive scratching, with few studies on psychoneuroimmunology.

Objective:

We aimed to estimate the levels of stress, depression, and anxiety, and to measure serum levels of neurotrophins in patients with lichen simplex chronicus, and to correlate these parameters with the severity of the disease and pruritus.

Methods:

Thirty-six patients with lichen simplex chronicus and 36 age- and sex-matched healthy controls were included. Each participant was administered the Hospital Anxiety and Depression Scale and Perceived Stress Scale questionnaires, along with a visual analog scale for pruritus. Levels of neurotrophins (brain-derived neurotrophic factor, neurotrophin-3, nerve growth factor, glial cell line-derived neurotrophic factor) were determined by ELISA assays.

Results:

The scores of Perceived Stress Scale-10, Hospital Anxiety and Depression Scale were statistically higher in patients (p < 0.05 for all). The serum levels of all neurotrophins were significantly lower in patients compared to healthy controls (p < 0.05 for all). Disease severity showed no correlation with all four neurotrophins. In linear regression models applied for increased visual analog scale-pruritus scores and disease severity these two variables were statistically significant predictors (p = 0.043).

Study limitations:

A direct causal relationship was not addressed.

Conclusion:

Lichen simplex chronicus patients are at risk of increased levels of stress, anxiety, depression, and present decreased levels of neurotrophins, that may suggest a role in the pathophysiology of this disorder.

KEYWORDS
Anxiety; Depression; Neurodermatitis; Psychodermatology

Introduction

Lichen Simplex Chronicus (LSC), or circumscribed neurodermatitis, is a common dermatological disorder characterized by lichenification of the skin due to excessive scratching and/or rubbing caused by the itch-scratch-itch cycle, which is hard to break. It has been estimated that LSC affects up to 12% of the total population.¹1 Lotti T, Buggiani G, Prignano F. Prurigo nodularis and lichen simplex chronicus. Dermatol Ther. 2008;21:42–6. Although some authors believe that it is a chronic and localized form of atopic dermatitis, its pathogenesis is still unclear. Previous reports indicate that psychological factors may play a role in the initiation of the disease and its persistence. Patients with LSC have proportionally higher incidences of depressive, dissociative, and anxiety disorders, obsessive-compulsive personality traits, sleep disturbances, and sexual dysfunction.²2 Konuk N, Koca R, Atik L, Muhtar S, Atasoy N, Bostanci B. Psychopathology, depression and dissociative experiences in patients with lichen simplex chronicus. Gen Hosp Psychiatry. 2007;29:232–5.^,³3 Martín-Brufau R, Corbalán-Berná J, Ramirez-Andreo A, Brufau-Redondo C, Limiñana-Gras R. Personality differences between patients with lichen simplex chronicus and normal population: A study of pruritus. Eur J Dermatol. 2010;20:359–63.^,⁴4 Liao YH, Lin CC, Tsai PP, Shen WC, Sung FC, Kao CH. Increased risk of lichen simplex chronicus in people with anxiety disorder: a nationwide population-based retrospective cohort study. Br J Dermatol. 2014;170:890–4.^,⁵5 Kouris A, Christodoulou C, Efstathiou V, Plarsidaki E, Tsatovidou R, Torlidi-Kordera E, et al. Comparative study of quality of life and obsessive-compulsive tendencies in patients with chronic hand eczema and Lichen Simplex Chronicus. Dermatitis. 2016;27:127–30. An increased likelihood of comorbid mental health disorders, including developmental, psychotic, and mood disorders, substance abuse, and cognitive disorders were reported in LSC.⁶6 Singam V, Patel KR, Silverberg JI. Association of prurigo nodularis and lichen simplex chronicus with hospitalization for mental health disorders in US adults. Arch Dermatol Res. 2020;312:587–93.

Skin is the largest, most innervated organ of the body, and the brain shares a common embryological origin with the ectoderm. The central nervous system (CNS) responds to psychological stress by activating the Hypothalamic-Pituitary-Adrenal axis (HPA axis) and autonomic nervous system and by modulating microglia at a local level. Neurotrophins, such as Brain-Derived Neurotrophic Factor (BDNF), Neurotrophin-3 (NT-3), Nerve Growth Factor (NGF), and Glial cell line-derived Neurotrophic Factor (GDNF), show neuroprotective effects in the CNS and play a crucial role in the growth, differentiation, maintenance, and synaptic plasticity of the neuronal and immune systems. Abnormalities in the levels of these neurotrophic factors may contribute to the dysfunction of astrocytes and microglia.⁷7 Oglodek EA, Just MJ, Szromek AR, Araszkiewicz A. Melatonin and neurotrophins NT-3, BDNF, NGF in patients with varying levels of depression severity. Pharmacol Rep. 2016;68:945–51. This may, in turn, directly create some alterations in the skin or induce the release of immunological or hormonal mediators that cause pathological changes in the skin by upsetting the balance of nervous system mediators.⁸8 Honeyman JF. Psychoneuroimmunology and the Skin. Acta Derm Venereol. 2016;96:38–46. Several studies have confirmed increased levels of NGF or BDNF in atopic dermatitis, chronic spontaneous urticaria, symptomatic dermographism, acne vulgaris patients with depressive symptoms, and uremic patients with pruritus.⁹9 Raap U, Goltz C, Deneka N, Bruder M, Renz H, Kapp A, et al. Brain-derived neurotrophic factor is increased in atopic dermatitis and modulates eosinophil functions compared with that seen in nonatopic subjects. J Allergy Clin Immunol. 2005;115:1268–75.^,¹⁰10 Papoiu ADP, Wang H, Nattkemper L, Tey HL, Ishiuji Y Yiong-Huak C. A study of serum concentrations and dermal levels of NGF in atopic dermatitis and healthy subjects. Neuropeptides. 2011;45:417–22.^,¹¹11 Rössing K, Novak N, Mommert S, Pfab F, Gehring M, Wedi B, et al. Brain-derived neurotrophic factor is increased in serum and skin levels of patients with chronic spontaneous urticaria. Clin Exp Allergy. 2011;41:1392–9.^,¹²12 Erpolat S, Celik HT, Bozkurt B. Brain-derived neurotrophic factor is increased in serum levels of patients with symptomatic dermographism. Postepy Dermatol Alergol. 2017;34:346–9.^,¹³13 He HY, Tian JL, Deng YQ, Xiong X, Xu Y Liao YM, et al. Association of brain-derived neurotrophic factor levels and depressive symptoms in young adults with acne vulgaris. BMC Psychiatry. 2019;19:193.^,¹⁴14 Sorour NE, Elesawy FM, Tabl HA, Ibrahim ME, Akl EM. Evaluation of serum levels of neurotrophin 4 and brain-derived nerve growth factor in uremic pruritus patients. Clin Cosmet Investig Dermatol. 2019;12:109–14.

The aim of the present study was to investigate depression, anxiety, quality of life, and perceived stress levels, and to measure serum neurotrophin levels in patients with LSC, and to determine whether there is a relationship between these parameters and the severity of symptoms.

Methods

This cross-sectional, case-control study was carried out between October 2019 and November 2020. Thirty-six patients diagnosed with LSC and 36 healthy age- and sex-matched subjects were included in the study. Individuals under 18 years old, with any other skin/systemic disease or mental disorder, or on any medication were excluded from the study. The study was approved by the ethics committee (nº 1347). All participants were given informed consent prior to participation and examined by the same dermatologists. Relevant investigations and/or skin biopsies were performed to confirm the diagnosis of LSC when indicated. The severity of the disease (mild, moderate, or severe) was recorded.¹⁵15 Pascoe VL, Enamandram M, Corey KC, Cheng CE, Javorsky EJ, Sung SM, et al. Using the Physician Global Assessment in a clinical setting to measure and track patient outcomes. JAMA Dermatol. 2015;151:375–81. The demographics, severity of the disease, and results of the Dermatology Life Quality Index (DLQI), HADS,¹⁶16 Cohen S, Williamson GE, Spacapan S, Oskamp SE. Perceived stress in a probability sample of the United States. In: J Appl Soc Psychol. Newbury Park: Sage; 1988. PSS-10, and VAS-Pruritus were recorded for each participant.¹⁶16 Cohen S, Williamson GE, Spacapan S, Oskamp SE. Perceived stress in a probability sample of the United States. In: J Appl Soc Psychol. Newbury Park: Sage; 1988.^,¹⁷17 Finlay AY, Khan GK. Dermatology Life Quality Index (DLQI) – a simple practical measure for routine clinical use. Clin Exp Dermatol. 1994;19:210–6. Serum IgE levels were determined using an automated chemiluminescence assay; NGF, NT-3, GDNF, and BDNF levels were determined using ELISA kits. Full details of the questionnaires, ELISA, and statistical analyses are attached in Supplementary materials.

Results

The demographics and disease characteristics of the study group are shown in Table 1. The mean age was 37.8 ± 11.9, and the most common localization was the back (n = 16. 44%). The PSS-10, HADS-A, and HADS-D scores were statistically higher in the LSC group. The laboratory parameters of all neurotrophins were significantly lower in the LSC group (Table 2). The mean values of serum IgE and the peripheral blood eosinophil count did not differ between groups. A correlation analysis showed that disease severity (r = 0.366, p = 0.028) and HADS-D score (r = 0.378, p = 0.023) correlated with the VAS-Pruritus score, whereas the HADS-A score correlated with disease severity (r = 0.358, p = 0.032). Disease severity showed no correlation with the serum levels of all four neurotrophins (p > 0.05 for all) (Table 3). Linear regression analyses to assess the contribution of the scores of all implemented questionnaires (HADS, PSS-10, DLQI) and the serum levels of neurotrophins as well as serum IgE and eosinophil counts to VAS-Pruritus scores and disease severity are shown in Tables 4 and 5. Disease severity was statistically associated with the VAS-Pruritus score ( p = 0.043 and ß = 0.396).

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Table 1
Demographic and clinical characteristics of the Lichen simplex chronicus (LSC) and control groups.

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Table 2
Comparison of questionnaire scores and laboratory parameters between Lichen simplex chronicus (LSC) and control groups.

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Table 3
Spearman’s correlation between VAS, disease severity, and study parameters.

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Table 4
Linear regression model for variables identified as significant for increased VAS-Pruritus score.

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Table 5
Linear regression model for variables identified as significant for disease severity.

Discussion

Our results showed increased stress, anxiety, and depression in LSC group compared to controls. Perceived stress refers to the feelings or thoughts that an individual has about how much stress they are under at a given point in time or over a given period. Theoretical definitions of stress highlight the role of perception as a crucial factor in its experience.¹⁸18 Gellman MD, Turner JR. Encyclopedia of behavioral medicine. New York: Springer; 2013. The PSS measures individuals’ perception of stress over the past month. The fact that patients with LSC had higher PSS scores than the controls support the idea that LSC patients have higher mental distress and thus that mental stress may play a role in LSC. Chronic stressors can promote psychoneuroimmunological changes via the HPA axis, resulting in an exacerbation of current skin conditions or the development of new ones. These conditions may impact one’s quality of life negatively, resulting in a decline in psychological well-being and an exacerbation of current psychiatric disorders or the formation of new ones. Additionally, high VAS-Pruritus scores (mean=7, min-max 6–9) were shown in LSC, that were correlated with disease severity and HADS-D scores. Therefore, the severity of itch, disease and depression played a role in the LSC process. Dalgard et al. reported that the presence of itch in dermatological patients was significantly associated with clinical depression, suicidal ideation, and stress in diverse countries.¹⁹19 Dalgard FJ, Svensson A, Halvorsen JA, Gieler U, Schut C, Tomas-Aragones L, et al. Itch and mental health in dermatological patients across Europe: a cross-sectional study in 13 countries. J Invest Dermatol. 2020;140:568–73. Yamamato et al. investigated the link between pruritic symptoms and psychological stress using PSS, and a relationship between the severity of pruritus and psychological symptoms was shown in the general population.²⁰20 Yamamoto Y Yamazaki S, Hayashino Y Takahashi O, Tokuda Y , Shimbo T et al. Association between frequency of pruritic symptoms and perceived psychological stress: a Japanese population-based study. Arch Dermatol. 2009;145:1384–8. Yalc¸in et al. found that 62% of 50 LSC patients had at least one psychiatric comorbidity, mostly major depressive disorder (32%), dysthymia (18%), and generalized anxiety disorder (12%).²¹21 Yalc¸in M, Bas A, Ergelen M, Gökce E, Saglam NGU, Bas TO. Psychiatric comorbidity and temperament-character traits of the patients with lichen simplex chronicus: The relation with the symptom severity of the disease. Dermatol Ther. 2020:e14389. Halvorsen et al. stated that itch is a greater risk factor for psychological problems compared to chronic eczema without itch.²²22 Halvorsen JA, Lien L, Dalgard F, Bjertness E, Stern RS. Suicidal ideation, mental health problems, and social function in adolescents with eczema: a population-based study. J Invest Dermatol. 2014;134:1847–54.

All these findings beg the question of whether the psychoneuroimmunological system plays any pathogenetic role in the relationship between itch and psychological stress and thus between LSC and psychological stress. After all, the neurological, endocrine and immune systems interact with each other to develop a sufficient stress response for the body and mind by utilizing a series of neurotrophins, neuropeptides, neurotransmitters, and neurohormones.

Neurotrophins belong to a family of trophic factors that regulate the survival, growth, and programmed cell death of neurons.²³23 Khan N, Smith MT. Neurotrophins and neuropathic pain: role in pathobiology. Molecules. 2015;20:10657–88. They exert immunomodulatory functions not only on nerves but also on immune cells, which was previously proven for NGF.²⁴24 Levi-Montalcini R, Dal Toso R, della Valle F, Skaper SD, Leon A. Update of the NGF saga. J Neurol Sci. 1995;130:119–27. Some neurotrophins were studied in different dermatological conditions.⁹9 Raap U, Goltz C, Deneka N, Bruder M, Renz H, Kapp A, et al. Brain-derived neurotrophic factor is increased in atopic dermatitis and modulates eosinophil functions compared with that seen in nonatopic subjects. J Allergy Clin Immunol. 2005;115:1268–75.^,¹⁰10 Papoiu ADP, Wang H, Nattkemper L, Tey HL, Ishiuji Y Yiong-Huak C. A study of serum concentrations and dermal levels of NGF in atopic dermatitis and healthy subjects. Neuropeptides. 2011;45:417–22.^,¹²12 Erpolat S, Celik HT, Bozkurt B. Brain-derived neurotrophic factor is increased in serum levels of patients with symptomatic dermographism. Postepy Dermatol Alergol. 2017;34:346–9.^,¹³13 He HY, Tian JL, Deng YQ, Xiong X, Xu Y Liao YM, et al. Association of brain-derived neurotrophic factor levels and depressive symptoms in young adults with acne vulgaris. BMC Psychiatry. 2019;19:193.^,¹⁴14 Sorour NE, Elesawy FM, Tabl HA, Ibrahim ME, Akl EM. Evaluation of serum levels of neurotrophin 4 and brain-derived nerve growth factor in uremic pruritus patients. Clin Cosmet Investig Dermatol. 2019;12:109–14. In several skin chronic inflammations, such as atopic dermatitis, psoriasis, and prurigo, NGF expression was increased in the lesions.²⁵25 Molina FA, Burrows NP, Jones RR, Terenghi G, Polak JM. Increased sensory neuropeptides in nodular prurigo: a quantitative immunohistochemical analysis. Br J Dermatol. 1992;127:344–51.^,²⁶26 Raychaudhuri SP, Raychaudhuri SK. Role of NGF and neurogenic inflammation in the pathogenesis of psoriasis. Progress in brain research. 2004;146:433–7.^,²⁷27 Cui S, Xiao T, Wang Y Lu H, Wang Y Gao XH, et al. Morphological relationship between nerve fibers and Langerhans cells in the epidermis of psoriasis vulgaris and lichen simplex chronicus. Journal of dermatological science. 2009;56:132–4. In fact, the number of peripheral nerve fibers and the concentration of NGF in LSC lesions have been reported to be higher. In the present study, it is noteworthy that all neurotrophins, including NT-3, NGF, GDNF, and BDNF, were significantly lower in LSC patients compared to healthy controls. This may mean that these declines were far from chance occurrences. Furthermore, neurotrophins, especially BDNF and NT-3, have been investigated in mood disorders and found to play a role in depression and anxiety.²⁸28 de Miranda AS, de Barros JLVM, Teixeira AL. Is neurotrophin-3 (NT-3): a potential therapeutic target for depression and anxiety? Expert Opin Ther Targets. 2020;24:1225–38. He et al. showed that serum BDNF levels were lower and negatively associated with depressive symptoms in young Chinese adults with acne vulgaris.¹³13 He HY, Tian JL, Deng YQ, Xiong X, Xu Y Liao YM, et al. Association of brain-derived neurotrophic factor levels and depressive symptoms in young adults with acne vulgaris. BMC Psychiatry. 2019;19:193. They also found that the severity of the disease was not related to depression scores in their acne patients, as did we in LSC. In the present study, all neurotrophins were no correlated with LSC severity.

Finally, LSC patients had increased levels of perceived stress, anxiety, and depression, and also decreased levels of neurotrophins, which play a significant role in brain and nerve chemistry. However, the question of which came first, LSC or these psychoneuroimmunological issues were not addressed. Decreased neurotrophin levels might lead to depression or anxiety and may trigger LSC, or conversely, LSC might cause depression or anxiety by reducing the quality of life, which may in turn decrease neurotrophins. It might even be a two-way relationship. These results may be used to help understand the disease better, shine a light on its pathogenesis, or discover new therapy options for LSC in the future.

Conclusion

The present study showed that LSC patients are at risk of increased levels of stress, anxiety, depression, impaired quality of life and decreased levels of neurotrophins. Decreased serum levels of neurotrophins may be directly related to the etiology of LSC or associated with the high percentage of psychiatric disorders in that patient population. Future studies are needed to address the psychoneuroimmunological basis of LSC and for new therapies.

☆
How to cite this article: Altunay İK, Özkur E, Ugurer E, Baltan E, Aydin Ç, Serin E. More than a skin disease: stress, depression, anxiety levels, and serum neurotrophins in lichen simplex chronicus. An Bras Dermatol. 2021;96:700–5.
☆☆
Study conducted at the Sisli Hamidiye Etfal Research and Training Hospital, Istanbul, Turkey.
Financial support

Health Sciences University, coordinatorship of scientific research projects.

References

¹
Lotti T, Buggiani G, Prignano F. Prurigo nodularis and lichen simplex chronicus. Dermatol Ther. 2008;21:42–6.
²
Konuk N, Koca R, Atik L, Muhtar S, Atasoy N, Bostanci B. Psychopathology, depression and dissociative experiences in patients with lichen simplex chronicus. Gen Hosp Psychiatry. 2007;29:232–5.
³
Martín-Brufau R, Corbalán-Berná J, Ramirez-Andreo A, Brufau-Redondo C, Limiñana-Gras R. Personality differences between patients with lichen simplex chronicus and normal population: A study of pruritus. Eur J Dermatol. 2010;20:359–63.
⁴
Liao YH, Lin CC, Tsai PP, Shen WC, Sung FC, Kao CH. Increased risk of lichen simplex chronicus in people with anxiety disorder: a nationwide population-based retrospective cohort study. Br J Dermatol. 2014;170:890–4.
⁵
Kouris A, Christodoulou C, Efstathiou V, Plarsidaki E, Tsatovidou R, Torlidi-Kordera E, et al. Comparative study of quality of life and obsessive-compulsive tendencies in patients with chronic hand eczema and Lichen Simplex Chronicus. Dermatitis. 2016;27:127–30.
⁶
Singam V, Patel KR, Silverberg JI. Association of prurigo nodularis and lichen simplex chronicus with hospitalization for mental health disorders in US adults. Arch Dermatol Res. 2020;312:587–93.
⁷
Oglodek EA, Just MJ, Szromek AR, Araszkiewicz A. Melatonin and neurotrophins NT-3, BDNF, NGF in patients with varying levels of depression severity. Pharmacol Rep. 2016;68:945–51.
⁸
Honeyman JF. Psychoneuroimmunology and the Skin. Acta Derm Venereol. 2016;96:38–46.
⁹
Raap U, Goltz C, Deneka N, Bruder M, Renz H, Kapp A, et al. Brain-derived neurotrophic factor is increased in atopic dermatitis and modulates eosinophil functions compared with that seen in nonatopic subjects. J Allergy Clin Immunol. 2005;115:1268–75.
¹⁰
Papoiu ADP, Wang H, Nattkemper L, Tey HL, Ishiuji Y Yiong-Huak C. A study of serum concentrations and dermal levels of NGF in atopic dermatitis and healthy subjects. Neuropeptides. 2011;45:417–22.
¹¹
Rössing K, Novak N, Mommert S, Pfab F, Gehring M, Wedi B, et al. Brain-derived neurotrophic factor is increased in serum and skin levels of patients with chronic spontaneous urticaria. Clin Exp Allergy. 2011;41:1392–9.
¹²
Erpolat S, Celik HT, Bozkurt B. Brain-derived neurotrophic factor is increased in serum levels of patients with symptomatic dermographism. Postepy Dermatol Alergol. 2017;34:346–9.
¹³
He HY, Tian JL, Deng YQ, Xiong X, Xu Y Liao YM, et al. Association of brain-derived neurotrophic factor levels and depressive symptoms in young adults with acne vulgaris. BMC Psychiatry. 2019;19:193.
¹⁴
Sorour NE, Elesawy FM, Tabl HA, Ibrahim ME, Akl EM. Evaluation of serum levels of neurotrophin 4 and brain-derived nerve growth factor in uremic pruritus patients. Clin Cosmet Investig Dermatol. 2019;12:109–14.
¹⁵
Pascoe VL, Enamandram M, Corey KC, Cheng CE, Javorsky EJ, Sung SM, et al. Using the Physician Global Assessment in a clinical setting to measure and track patient outcomes. JAMA Dermatol. 2015;151:375–81.
¹⁶
Cohen S, Williamson GE, Spacapan S, Oskamp SE. Perceived stress in a probability sample of the United States. In: J Appl Soc Psychol. Newbury Park: Sage; 1988.
¹⁷
Finlay AY, Khan GK. Dermatology Life Quality Index (DLQI) – a simple practical measure for routine clinical use. Clin Exp Dermatol. 1994;19:210–6.
¹⁸
Gellman MD, Turner JR. Encyclopedia of behavioral medicine. New York: Springer; 2013.
¹⁹
Dalgard FJ, Svensson A, Halvorsen JA, Gieler U, Schut C, Tomas-Aragones L, et al. Itch and mental health in dermatological patients across Europe: a cross-sectional study in 13 countries. J Invest Dermatol. 2020;140:568–73.
²⁰
Yamamoto Y Yamazaki S, Hayashino Y Takahashi O, Tokuda Y , Shimbo T et al. Association between frequency of pruritic symptoms and perceived psychological stress: a Japanese population-based study. Arch Dermatol. 2009;145:1384–8.
²¹
Yalc¸in M, Bas A, Ergelen M, Gökce E, Saglam NGU, Bas TO. Psychiatric comorbidity and temperament-character traits of the patients with lichen simplex chronicus: The relation with the symptom severity of the disease. Dermatol Ther. 2020:e14389.
²²
Halvorsen JA, Lien L, Dalgard F, Bjertness E, Stern RS. Suicidal ideation, mental health problems, and social function in adolescents with eczema: a population-based study. J Invest Dermatol. 2014;134:1847–54.
²³
Khan N, Smith MT. Neurotrophins and neuropathic pain: role in pathobiology. Molecules. 2015;20:10657–88.
²⁴
Levi-Montalcini R, Dal Toso R, della Valle F, Skaper SD, Leon A. Update of the NGF saga. J Neurol Sci. 1995;130:119–27.
²⁵
Molina FA, Burrows NP, Jones RR, Terenghi G, Polak JM. Increased sensory neuropeptides in nodular prurigo: a quantitative immunohistochemical analysis. Br J Dermatol. 1992;127:344–51.
²⁶
Raychaudhuri SP, Raychaudhuri SK. Role of NGF and neurogenic inflammation in the pathogenesis of psoriasis. Progress in brain research. 2004;146:433–7.
²⁷
Cui S, Xiao T, Wang Y Lu H, Wang Y Gao XH, et al. Morphological relationship between nerve fibers and Langerhans cells in the epidermis of psoriasis vulgaris and lichen simplex chronicus. Journal of dermatological science. 2009;56:132–4.
²⁸
de Miranda AS, de Barros JLVM, Teixeira AL. Is neurotrophin-3 (NT-3): a potential therapeutic target for depression and anxiety? Expert Opin Ther Targets. 2020;24:1225–38.

Publication Dates

Publication in this collection
17 Jan 2022
Date of issue
Nov-Dec 2021

History

Received
11 Mar 2021
Accepted
16 Apr 2021
Published
04 Oct 2021

This is an Open Access article distributed under the terms of the Creative Commons Attribution License, which permits unrestricted use, distribution, and reproduction in any medium, provided the original work is properly cited.

[1] ☆
How to cite this article: Altunay İK, Özkur E, Ugurer E, Baltan E, Aydin Ç, Serin E. More than a skin disease: stress, depression, anxiety levels, and serum neurotrophins in lichen simplex chronicus. An Bras Dermatol. 2021;96:700–5.

[2] ☆☆
Study conducted at the Sisli Hamidiye Etfal Research and Training Hospital, Istanbul, Turkey.

[3] Financial support

Health Sciences University, coordinatorship of scientific research projects.

		LSC (n = 36)	Controls (n = 36)	p
Sex, n (%)	Male	7 (19.4)	7 (19.4)	1.000
	Female	29 (80.6)	29 (80.6)
Age (yrs) Mean ± SD (Min-Max)		37.8 ± 11.9 (19–59)	37.8 ± 11.9 (19–59)	1.000
Marital status, n (%)	Single	15 (41.7)	13 (36.1)	.635
	Married/cohabitating	20 (55.6)	23 (63.9)
	Divorced/widowed/separated	1 (2.8)	0 (0.0)
Disease duration (yrs.) Median (IQR)		3 (1–7)
VAS-Pruritus Median (IQR)		7 (6–9)
DLQI Median (IQR)		4.5 (3–13)
Disease severity, n (%)	Mild	10 (27.7)
	Moderate	14 (38.8)
	Severe	12 (33.3)
Localization, n (%)	Head	4 (11.1)
	Front chest	4 (11.1)
	Back	16 (44.4)
	Upper extremities	5 (13.9)
	Lower extremities	13 (36.1)
	Gluteus	8 (22.2)

	LSC Mean ± SD (Min-Max)	Controls Mean ± SD (Min-Max)	p
PSS-10	18.3 ± 6.4 (0–28)	12.6 ± 5.1 (2–23)	< 0.001
HADS-A	8.28 ± 4.65 (1–19)	5.28 ± 2.94 (0–10)	0.002
HADS-D	7.39 ± 4.93 (0–20)	4.17 ± 2.48 (0–13)	0.001
	Median (IQR)	Median (IQR)
IgE (mg/dL)	36.7 (8.3–121)	58.1 (21.2–100)	0.374
Eosinophils (×106/mL)	0.13 (0.06–0.27)	0.12 (0.08–0.18)	0.969
NGF (ng/mL)	141.7 (80.3–689.9)	437 (148.4–1,142.0)	0.010
GDNF (ng/mL)	1.61 (0.88–11.63)	5.24 (1.80–20.26)	0.019
NT (pmoL/L)	49 (27.1–143.1)	98.2 (47.2–242)	0.012
BDNF (ng/mL)	0.88 (0.71–1.87)	1.34 (0.92–2.43)	0.004

	VAS-Pruritus		Disease Severity
	r	p	r	p
Disease severity	0.366	0.028
Age (yrs)	-0.088	0.610	-0.031	0.857
Disease duration (yrs)	-0.019	0.912	0.266	0.116
DLQI	0.319	0.058	0.359	0.031
PSS-10	0.231	0.175	0.218	0.201
HADS-A	0.309	0.067	0.358	0.032
HADS-D	0.378	0.023	0.107	0.536
IgE (mg/dL)	0.203	0.234	0.118	0.494
Eosinophils (×106/mL)	0.132	0.442	0.069	0.689
NGF (ng/mL)	-0.055	0.748	-0.103	0.548
GDNF (ng/mL)	-0.055	0.750	-0.135	0.433
NT (pmoL/L)	-0.020	0.906	-0.073	0.673
BDNF (ng/mL)	0.016	0.925	-.030	0.863

Model	Unstandardized Coefficients B	Standardized Coefficients ß	p
Constant	2.978
Disease severity	0.376	0.396	0.043
Sex	-1.154	-0.206	0.290
Age	-0.027	-0.144	0.481
DLQI	0.061	0.151	0.395
PSS-10	-0.019	-0.055	0.841
HADS-A	0.088	0.182	0.444
HADS-D	0.168	0.369	0.133
IgE	-0.001	-0.246	0.146
Eosinophils	1.596	0.110	0.550
NGF	0.000	0.131	0.769
GDNF	0.032	0.310	0.340
NT	0.002	0.356	0.319
BDNF	1.634	0.688	0.393

Model 1	Unstandardized Coefficients B	Standardized Coefficients ß	p
Constant	0.970
VAS	0.480	0.455	0.043
Sex	0.820	0.139	0.509
Age	0.007	0.036	0.870
DLQI	0.059	0.138	0.470
PSS-10	0.044	0.118	0.685
HADS-A	0.094	0.184	0.471
HADS-D	-0.205	-0.427	0.103
IgE	0.002	0.302	0.093
Eosinophils	-1.151	-0.076	0.703
NGF	-0.002	-0.420	0.377
GDNF	-0.027	-0.251	0.472
NT	0.000	0.053	0.891
BDNF	1.144	0.457	0.599

Brasil

Brasil

Abstract

Background:

Objective:

Methods:

Results:

Study limitations:

Conclusion:

Introduction

Methods

Results

Discussion

Conclusion

References

Publication Dates

History