Nail abnormalities in patients with vitiligo

Topal, Ilteris Oguz; Gungor, Sule; Kocaturk, Ozgur Emek; Duman, Hatice; Durmuscan, Mustafa

doi:10.1590/abd1806-4841.20164620

Abstract:

Background:

Vitiligo is an acquired pigmentary skin disorder affecting 0.1-4% of the general population. The nails may be affected in patients with an autoimmune disease such as psoriasis, and in those with alopecia areata. It has been suggested that nail abnormalities should be apparent in vitiligo patients.

Objective:

We sought to document the frequency and clinical presentation of nail abnormalities in vitiligo patients compared to healthy volunteers. We also examined the correlations between nail abnormalities and various clinical parameters.

Methods:

This study included 100 vitiligo patients and 100 healthy subjects. Full medical histories were collected from the subjects, who underwent thorough general and nail examinations. All nail changes were noted. In the event of clinical suspicion of a fungal infection, additional mycological investigations were performed.

Results:

Nail abnormalities were more prevalent in the patients (78%) than in the controls (55%) (p=0.001). Longitudinal ridging was the most common finding (42%), followed by (in descending order): leukonychia, an absent lunula, onycholysis, nail bed pallor, onychomycosis, splinter hemorrhage and nail plate thinning. The frequency of longitudinal ridging was significantly higher in patients than in controls (p<0.001).

Conclusions:

Nail abnormalities were more prevalent in vitiligo patients than in controls. Systematic examination of the nails in such patients is useful because nail abnormalities are frequent. However, the causes of such abnormalities require further study. Longitudinal ridging and leukonychia were the most common abnormalities observed in this study.

Keywords:
Nails; Onycholysis; Vitiligo

INTRODUCTION

Nail features are important in dermatology; various abnormalities are apparent in patients with dermatological disorders, including psoriasis, lichen planus, and alopecia areata.¹1 Holzberg M. Common nail disorders. Dermatol Clin. 2006;24:349-54. Neither the frequency nor the nature of nail abnormalities in vitiligo is known.

Vitiligo is an acquired pigmentary disorder, characterized by a loss of melanocytes, resulting in the appearance of white spots, or leukoderma. Vitiligo affects 0.1-4% of the global population.²2 Handa S, Dogra S. Epidemiology of childhood vitiligo: a study of 625 patients from north India. Pediatr Dermatol. 2003;20:207-10. Recent clinical studies support the notion that vitiligo is associated with autoimmune disorders, particularly Hashimoto's thyroiditis and Graves' disease; other endocrinopathies, including Addison's disease and diabetes mellitus; alopecia areata; pernicious anemia; and inflammatory bowel disease.³3 Akay BN, Bozkir M, Anadolu Y, Gullu S. Epidemiology of vitiligo, associated autoimmune diseases and audiological abnormalities: Ankara study of 80 patients in Turkey. J Eur Acad Dermatol Venereol. 2010;24:1144-50. Nail abnormalities are evident in 10-66% of patients with alopecia areata.⁴4 Kasumagic-Halilovic E, Prohic A. Nail changes in alopecia areata: frequency and clinical presentation. J Eur Acad Dermatol Venereol. 2009;23:240-1. The nails may be attacked by the same inflammatory cells that target the hair follicles of alopecia areata patients. The presumed autoimmune etiology of vitiligo, and the association between vitiligo and alopecia areata, support the hypothesis that nail abnormalities should be apparent in vitiligo patients.⁵5 Anbar T, Hay RA, Abdel-Rahman AT, Moftah NH, Al-Khayyat MA.Clinical study of nail changes in vitiligo. J Cosmet Dermatol. 2013;12:67-72.

Our aim was to determine the frequencies and types of nail abnormalities in vitiligo patients compared to normal, healthy volunteers.

METHODS

We conducted an open, non-randomized, paired, controlled clinical study featuring intentional sampling of vitiligo patients who visited the outpatient clinic at our Dermatology Department between December 2013 and January 2015. One hundred vitiligo patients were included. For each subject, we recorded the age, sex, clinical features of the disease, and disease duration. Vitiligo was usually clinically diagnosed; if necessary, skin biopsy material was subjected to histopathological examinations. Both fingernails and toenails were analyzed, and abnormalities noted. Additional mycological investigations were performed on patients with nail abnormalities suggesting a fungal infection. Other causes of such abnormalities, including congenital and traumatic dystrophy, were eliminated, while patients with thyroid, systemic, or other autoimmune diseases, were excluded.

The control group consisted of 100 age- and sex-matched healthy volunteers without a systemic or autoimmune disease, alopecia areata, or vitiligo; no volunteer took any medication for one month prior to the study.

The following were measured in all patients and controls: levels of hemoglobin, iron, vitamin B12, folic acid, blood glucose, anti-thyroglobulin antibodies, anti-thyroidperoxidase antibodies, thyroid stimulating hormone, free tri-iodothyronine, and free thyroxine; the concentrations of anti-hepatitis B, anti-hepatitis C, and anti-HIV antibodies; as well as the erythrocyte sedimentation rate.

This study was approved by the Ethics Committee of the Okmeydani Training and Research Hospital (Istanbul, Turkey).

Statistical comparisons featured chi-square testing and Spearman's correlation analysis. A p-value <0.05 was considered to reflect statistical significance.

RESULTS

In total, 51 patients (51%) were female and 49 (51%) were male; they ranged in age from 3-78 years (mean: 34.9±16.8 years; table 1). Most patients had focal vitiligo (39%), followed by acrofacial (30%), generalized (27%) and universal vitiligo (4%). The age at onset ranged from 3-73 years. Disease duration varied from 1 month to 39 years (mean: 4.9±6.7 years). The following nail abnormalities were present in 78 (78%) patients with vitiligo: longitudinal ridging (42%), leukonychia (16%), an absent lunula (13%), nail bed pallor (5%), onycholysis (5%), onychomycosis (5%), splinter hemorrhage (5%), nail plate thinning (4%), and clubbing (4%). Nail abnormalities were most frequent in patients with focal vitiligo (39%), followed by acrofacial (30%) and generalized vitiligo (27%).

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Table 1
Demographic data of patients and controls and the frequency of nail changes in them

The clinical features of the nail abnormalities in the controls and patients are listed in table 2. In the controls, longitudinal ridging, leukonychia, and an absent lunula, were the most common abnormalities, followed by onycholysis and nail bed pallor.

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Table 2
Clinical manifestations of the nail abnormalities among patients and controls

Nail abnormalities were significantly more frequent in vitiligo patients (78%) than in controls (55%) (p=0.001). Similarly, longitudinal ridging (Figure 1)was significantly more common among vitiligo patients than in controls (p<0.001).

Figure 1
Longitudinal ridging on the nails of a vitiligo patient

We found no correlation between the presence of nail abnormalities and patient age or vitiligo duration (p=0.150 and 0.357, respectively; Table 3).

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Table 3
Correlation between the presence of nail abnormalities and patient age or disease duration

DISCUSSION

Vitiligo is an acquired idiopathic disorder characterized by circumscribed, depigmented maculae and white patches. Functional melanocytes disappear from the involved skin; however, the mechanism remains unknown.⁶6 Di Chiacchio NG, Ferreira FR, de Alvarenga ML, Baran R. Nail trichrome vitiligo: case report and literature review. Br J Dermatol. 2013;168:668-9.^,⁷7 Ezzedine K, Lim HW, Suzuki T, Katayama I, Hamzavi I, Lan CC,et al. Revised classification/nomenclature of vitiligo and related issues: the Vitiligo Global Issues Consensus Conference. Pigment Cell Melanoma Res. 2012;25:E1-13. Recent studies have suggested that autoimmunity plays a role in the pathogenesis of vitiligo. Further, both cellular and humoral immunity have been implicated in the development of vitiligo, as studies continue to be conducted.⁸8 Sandoval-Cruz M, García-Carrasco M, Sánchez-Porras R, Mendoza-Pinto C, Jiménez-Hernández M, Munguía-Realpozo P, et al. Immunopathogenesis of vitiligo. Autoimmun Rev. 2011;10:762-5. Nail abnormalities may develop in patients with autoimmune disorders, including psoriasis. Abnormalities are common (10-66%) in patients with alopecia areata, and are also evident in >5% of patients with autoimmune thyroiditis. Thus, the apparent associations may be real. It has been hypothesized that nail abnormalities should be apparent in vitiligo patients.⁴4 Kasumagic-Halilovic E, Prohic A. Nail changes in alopecia areata: frequency and clinical presentation. J Eur Acad Dermatol Venereol. 2009;23:240-1.^,⁹9 Barth JH, Telfer NR, Dawber RP. Nail abnormalities and autoimmunity. J Am Acad Dermatol. 1988;18:1062-5.

Anectodal reports of nail abnormalities in vitiligo patients have appeared. Such abnormalities were first reported by Milligan et al.¹⁰10 Milligan A, Barth JH, Graham-Brown RA, Dawber RP. Pseudo-mycotic nail dystrophy and vitiligo. Clin Exp Dermatol. 1988;13:109-10. in two vitiligo patients. Pseudo-mycotic nail dystrophy was evident and in both cases, all nails were uniformly involved (the"twenty-nails syndrome"). Later, Peloro¹¹11 Peloro TM, Pride HB. Twenty-nail dystrophy and vitiligo: a rare association. J Am Acad Dermatol. 1999;40:488-90. described "twenty-nail dystrophy" with vitiligo in a 10-year-old female. An association between twenty-nail dystrophy (trachyonychia) and vitiligo was suggested by Barth et al.⁹9 Barth JH, Telfer NR, Dawber RP. Nail abnormalities and autoimmunity. J Am Acad Dermatol. 1988;18:1062-5. in 1988; these authors described eight patients with both vitiligo and nail abnormalities, including trachyonychia, pitting, onycholysis, atrophy, and pseudo-mycotic changes. Two patients had additional autoimmune disorders, and onycholysis was apparent. The detailed pathogenesis of twenty-nail dystrophy remains unknown; the condition is sometimes idiopathic, but it may occur in association with other disorders.¹¹11 Peloro TM, Pride HB. Twenty-nail dystrophy and vitiligo: a rare association. J Am Acad Dermatol. 1999;40:488-90. Kandpur et al. described three vitiligo patients who developed twenty-nail dystrophy.¹²12 Khandpur S, Reddy BS. An association of twenty-nail dystrophy with vitiligo.J Dermatol. 2001;28:38-42. Nail matrix biopsies revealed focal lichenoid reactions and chronic inflammatory infiltrates in the dermal papillae and around the blood vessels. It was suggested that the association between vitiligo and twenty-nail dystrophy could be explained by the autoimmune origins of both disorders.¹³13 Khandpur S, Bansal A, Sharma VK, Bhatti SS, Singh MK. Twenty nail dystrophy in vitiligo. J Dermatol. 2007;34:189-92.

The literature on vitiligo patients' nails is confined to a single report on abnormalities in 79% of these patients. Longitudinal ridging and an absent lunula were significantly more common in patients than controls. The clinical form of vitiligo associated with nail involvement is principally non-segmental (71%), followed by segmental (53.3%).⁵5 Anbar T, Hay RA, Abdel-Rahman AT, Moftah NH, Al-Khayyat MA.Clinical study of nail changes in vitiligo. J Cosmet Dermatol. 2013;12:67-72. We studied 100 patients with non-segmental vitiligo. Nail abnormalities were evident in 39 patients (39%) with focal, 30 (30%) with acrofacial, and 27 (27%) with generalized, vitiligo. Of the vitiligo patients, 78% exhibited at least one nail abnormality. Some associations were similar to those noted in the only prior study (p=0.001). The most common abnormality was longitudinal ridging, apparent in 42% of patients, followed by leukonychia (16%) and the absence of a lunula (13%). Nail abnormalities were not associated with abnormalities of the hands or feet.

The most common nail abnormality was longitudinal ridging (42% of patients; such ridging presents as a series of superficial, narrow, longitudinal, parallel striations on the nail plate). The prevalance was 2.3% at one podiatry clinic. Ridging can develop in patients with psoriasis and lichen planus, and upon trauma or aging.¹⁴14 Bodman MA. Nail dystrophies. Clin Podiatr Med Surg. 2004;21:663-87. Our vitiligo patients were more frequently affected than the general podiatric populations. However, the pathogenesis remains unclear; thus, further study is needed.

The second most common nail abnormality was leukonychia (16%). White spots (leukonychia punctata) are usually attributable to trauma, which is known to trigger vitiligo. Earlier studies of the nails of alopecia areata patients indicated that punctate leukonychia may be attributable to focal involvement of the distal matrix.¹⁵15 Tosti A, Morelli R, Bardazzi F, Peluso AM. Prevalence of nail abnormalities in children with alopecia areata. Pediatr Dermatol. 1994;11:112-5.

Lunulas (the visible regions of the nail matrix ) were absent in 13% of our patients. This is the most frequent nail abnormality seen in hemodialysis patients, and has been attributed to anemia caused by chronic renal failure.¹⁵15 Tosti A, Morelli R, Bardazzi F, Peluso AM. Prevalence of nail abnormalities in children with alopecia areata. Pediatr Dermatol. 1994;11:112-5. Other common nail abnormalities in our patients were onycholysis, splinter hemorrhage, onychomycosis, and nail plate pallor.

CONCLUSION

Nail abnormalities were evident in our vitiligo patients. Vitiligo is an autoimmune disease; immune responses are abnormal, especially the roles played by T lymphocytes. The nails may be subject to an autoimmune attack, triggering nail abnormalities. Nail involvement was common among our patients with vitiligo. Longitudinal ridging and leukonychia were the most common abnormalities.

*
Work performed at the Department of Dermatology, Okmeydani Training and Research Hospital - Istanbul, Turkey.
Financial Support: None.

REFERENCES

¹
Holzberg M. Common nail disorders. Dermatol Clin. 2006;24:349-54.
²
Handa S, Dogra S. Epidemiology of childhood vitiligo: a study of 625 patients from north India. Pediatr Dermatol. 2003;20:207-10.
³
Akay BN, Bozkir M, Anadolu Y, Gullu S. Epidemiology of vitiligo, associated autoimmune diseases and audiological abnormalities: Ankara study of 80 patients in Turkey. J Eur Acad Dermatol Venereol. 2010;24:1144-50.
⁴
Kasumagic-Halilovic E, Prohic A. Nail changes in alopecia areata: frequency and clinical presentation. J Eur Acad Dermatol Venereol. 2009;23:240-1.
⁵
Anbar T, Hay RA, Abdel-Rahman AT, Moftah NH, Al-Khayyat MA.Clinical study of nail changes in vitiligo. J Cosmet Dermatol. 2013;12:67-72.
⁶
Di Chiacchio NG, Ferreira FR, de Alvarenga ML, Baran R. Nail trichrome vitiligo: case report and literature review. Br J Dermatol. 2013;168:668-9.
⁷
Ezzedine K, Lim HW, Suzuki T, Katayama I, Hamzavi I, Lan CC,et al. Revised classification/nomenclature of vitiligo and related issues: the Vitiligo Global Issues Consensus Conference. Pigment Cell Melanoma Res. 2012;25:E1-13.
⁸
Sandoval-Cruz M, García-Carrasco M, Sánchez-Porras R, Mendoza-Pinto C, Jiménez-Hernández M, Munguía-Realpozo P, et al. Immunopathogenesis of vitiligo. Autoimmun Rev. 2011;10:762-5.
⁹
Barth JH, Telfer NR, Dawber RP. Nail abnormalities and autoimmunity. J Am Acad Dermatol. 1988;18:1062-5.
¹⁰
Milligan A, Barth JH, Graham-Brown RA, Dawber RP. Pseudo-mycotic nail dystrophy and vitiligo. Clin Exp Dermatol. 1988;13:109-10.
¹¹
Peloro TM, Pride HB. Twenty-nail dystrophy and vitiligo: a rare association. J Am Acad Dermatol. 1999;40:488-90.
¹²
Khandpur S, Reddy BS. An association of twenty-nail dystrophy with vitiligo.J Dermatol. 2001;28:38-42.
¹³
Khandpur S, Bansal A, Sharma VK, Bhatti SS, Singh MK. Twenty nail dystrophy in vitiligo. J Dermatol. 2007;34:189-92.
¹⁴
Bodman MA. Nail dystrophies. Clin Podiatr Med Surg. 2004;21:663-87.
¹⁵
Tosti A, Morelli R, Bardazzi F, Peluso AM. Prevalence of nail abnormalities in children with alopecia areata. Pediatr Dermatol. 1994;11:112-5.

Publication Dates

Publication in this collection
Jul-Aug 2016

History

Received
07 Apr 2015
Accepted
03 Aug 2015

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

[1] *
Work performed at the Department of Dermatology, Okmeydani Training and Research Hospital - Istanbul, Turkey.

[2] Financial Support: None.

	Patients	Controls
Age (range), Mean±SD (years)	32 (3–78), 34.9±16.8	31.5 (3–78), 34.8±17.2
Sex (females/males)	51/49	50/50
Disease duration, mean±SD (months)	1–39, 4.9±6.7
Nail abnormalities
Present	78 (78%)	55 (55%) p=0.001
Absent	22 (22%)	45 (45%)

Nail abnormality	Number of controls (%)	Number of patients (%)	p-value
Longitudinal ridging	13 (13%)	42 (42%)	<0.001^a a Pearson’s chi-square test;
Leukonychia	13 (13%)	16 (16%)	0.688^b b Yates’ [corrected] chi-square test;
An absent lunula	13 (13%)	13 (13%)	1.000^b b Yates’ [corrected] chi-square test;
Onycholysis	2 (2%)	5 (5%)	0.445^c c Fisher’s exact chi-square test.
Nail plate pallor (pale nail)	5 (5%)	5 (5%)	1.000^b b Yates’ [corrected] chi-square test;
Splinter hemorrhage	1 (1%)	5 (5%)	0.212^c c Fisher’s exact chi-square test.
Onychomycosis	7 (7%)	5 (5%)	0.766^b b Yates’ [corrected] chi-square test;
Nail plate thinning	0	4 (4%)	0.121^c c Fisher’s exact chi-square test.
Clubbing	1 (1%)	4 (4%)	0.369^c c Fisher’s exact chi-square test.
Transverse ridging	2 (2%)	3 (3%)	1.000^c c Fisher’s exact chi-square test.
Nail plate thickening	0	2 (2%)	0.497^c c Fisher’s exact chi-square test.
Half-and-half nails	1 (1%)	2 (2%)	1.000^c c Fisher’s exact chi-square test.
Bright nail plate	2 (2%)	2 (2%)	1.000^c c Fisher’s exact chi-square test.
Longitudinal pigmentation	1 (1%)	1 (1%)	1.000^c c Fisher’s exact chi-square test.
Koilonychia	0	1 (1%)	1.000^c c Fisher’s exact chi-square test.
Terry nail	0	1 (1%)	1.000^c c Fisher’s exact chi-square test.
Thickening of the cuticle	0	1 (1%)	1.000^c c Fisher’s exact chi-square test.
Pitting	1 (1%)	1 (1%)	1.000^c c Fisher’s exact chi-square test.
Pterygium	1 (1%)	0	1.000^c c Fisher’s exact chi-square test.
Total number of nail abnormalities	100	100

	Prevalence of nail abnormalities
	r	p
Age (years)	0.145	0.150
Disease duration (years)	-0.093	0.357

Brasil

Brasil

Nail abnormalities in patients with vitiligo^* * Work performed at the Department of Dermatology, Okmeydani Training and Research Hospital - Istanbul, Turkey.

Abstract:

Background:

Objective:

Methods:

Results:

Conclusions:

INTRODUCTION

METHODS

RESULTS

DISCUSSION

CONCLUSION

REFERENCES

Publication Dates

History

Brasil

Brasil

Nail abnormalities in patients with vitiligo* * Work performed at the Department of Dermatology, Okmeydani Training and Research Hospital - Istanbul, Turkey.

Abstract:

Background:

Objective:

Methods:

Results:

Conclusions:

INTRODUCTION

METHODS

RESULTS

DISCUSSION

CONCLUSION

REFERENCES

Publication Dates

History

Nail abnormalities in patients with vitiligo^* * Work performed at the Department of Dermatology, Okmeydani Training and Research Hospital - Istanbul, Turkey.