Yellow nail syndrome: a review

The first case of yellow nail syndrome (YNS; OMIM 153300, ORPHA662) was probably reported by Heller in 1927 [1], but Samman & White described the first series of patients who had yellow nails associated with lymphedema in 1964 [2]. That report included 13 patients (six men, seven women; age range at onset 25–65 years), all of whom had very slow measured nail growth associated with abnormal nail-plate discoloration, ranging from pale yellow to dark greenish, and frequent onycholysis. Eight of them had ankle edema; one patient each had facial edema or Milroy’s disease (familial form of primary lymphedema). Four patients’ limb lymphangiograms showed lymphatic abnormalities, such as tortuous, dilated or hypoplastic vessels, which the authors considered suggestive of lymphatic dysfunction or defective lymph drainage being responsible for YNS. In this review, we analyze the available literature on this subject, describing clinical characteristics, explorations, associated diseases and management of this rare syndrome.

The literature search of the PubMed database used the words “yellow nail syndrome” for articles written in English or French. Other references cited in the identified articles were also considered.

YNS is characterized by a triad of thickened yellow nails, primary lymphedema and respiratory manifestations. It is an acquired condition of unknown etiology. It is a syndrome – not a disease – that is associated with conditions as different as diseases implicating the lymphatic system, autoimmune diseases or cancers. Whereas Samman & White’s first description of YNS included only nail discoloration, Emerson added pleural effusion to the diagnostic criteria [3]. Among the three clinical YNS characteristics (yellow nail syndrome, respiratory tract involvement, lymphedema), only two are required to diagnose YNS but it is difficult to call the entity YNS without nail abnormality [4]. Moreover, the three components are not necessarily present simultaneously, and may appear individually and sequentially, thereby making YNS diagnosis difficult. The complete triad is present only in 27–60% of the patients [5‐10] (Table 1). The percentage differences of a given clinical manifestation may be attributed to the medical specialty that recruited the patients.

No precise data are available to determine the exact prevalence of YNS, as fewer than 400 cases have been published in the literature, with an estimated prevalence <1/1,000,000. Cases have been described in all countries worldwide. YNS most often occurs in adults over 50 years old, with no sex predominance [5‐7]. Pediatric forms are very rarely reported [11‐21]: YNS may be present at birth (congenital) or develop before the age of 10 years [8].

A familial form of YNS has very rarely been described [5, 22‐24], affecting two siblings [25, 26] or a family with eight cases in four sibships over two generations [22]. The very few reported familial cases mimic a dominant inheritance pattern, which is not supported by any genetic evidence [5]. YNS may be associated with intellectual disability, in which case it evokes a more complex syndrome [25] or occurs in cases of consanguinity [17].

Although YNS etiology of remains unknown, some hypotheses were advanced. Lymphatic involvement is often evoked to explain lymphedema, pleural effusion (particularly chylothorax) or nail discoloration but it is difficult to implicate it in bronchiectasia and sinusitis. Lymphatic impairment is not easy to confirm. Four YNS patients underwent lower limb direct lymphangiography, less used at present, but lymphatic abnormalities were noted only in the patient with severe lymphedema. Quantitative limb lymphoscintigraphy with ^99mTc-colloidal antimony sulfide revealed less activity (percentage uptake) in the draining lymph nodes (inguinofemoral or axillary) [41]. Moreover, the uptake percentages in the axillary/inguinal lymph nodes of the YNS group were significantly lower than those of the normal controls but significantly higher than those of subjects with primary or secondary lymphedema, hence more suggestive of impaired lymph transport than the lymphatic hypoplasia/aplasia seen in true primary lymphedema. Furthermore, the YNS group without lower limb edema had better lymphatic drainage than those with edema [42] (Fig. 4). Maldonado et al. thought that YNS pathophysiology might be attributable to microvasculopathy associated with protein leakage rather than functional lymphatic impairment [43]. Notably, nailfold capillaroscopy occasionally showed dilated and tortuous capillary loops [44].

Defective lymphatic drainage might be responsible for the slow growth and thickened nails observed in YNS, and may reflect subungual tissue sclerosis leading to lymphatic obstruction. Light microscopy examination of sections of nail-matrix tissue revealed replacement of the normally loose fibrovascular subungual stroma by dense, fibrous tissue (composed of dense collagen deposits) extending from the immediate subepithelial stroma to a depth of 2.5 mm. Numerous ectatic, endothelium-lined channels were prominent within the fibrotic stroma [45]. Fibrosis and dilated lymphatic vessels were also seen in the parietal pleura of a YNS patient [46, 47]. The accumulation of lipofuscin pigment was advanced to explain the yellow discoloration [48], whereas abnormal nail keratinization might be explained by the presence electron microscopy-visualized keratohyalin granules, not found in normal adult nails.

More recently, it was hypothesized that titanium, especially titanium dioxide, might play a role in YNS. High titanium levels (determined by energy dispersive X-ray fluorescence) were detected in the nails of YNS patients but not in control nails. The authors postulated that titanium ions were released from titanium implants (inlays, crown) in the teeth or jaws through the galvanic action of amalgam or localized oxidative action of fluorides [49‐51]. Other sources of titanium ions were also suggested: joint implants, surgical staples, foods (chewing gum to try to explain YNS in children), medication excipients, cosmetics (sunscreen, moisturizers, shampoo, toothpaste) [50, 52]. Titanium’s hypothetical role remains possible, but probably not sufficient, because its presence in other organs (liver, spleen, lymph nodes, lung) of autopsied patients was not accompanied with nail yellowing [53].

Several infants had YNS associated with non-immune hydrops fetalis; this association is probably not fortuitous [54]. Non-immune hydrops fetalis was present at birth [20, 55]. A child with YNS had a brother who died of non-immune hydrops fetalis, suggesting a possible relationship between the two diseases [17].

YNS is very rarely associated with primary intestinal lymphangiectasia (Waldmann’s disease) (OMIM 152800, ORPHA90362) or lymphedema–distichiasis syndrome (OMIM 153400, ORPHA33001), suggesting that these entities have overlapping characteristics, including lymphatic impairment [56, 57]. Waldmann’s disease is characterized by primary intestinal lymphangiectasia, with lymph leakage into the bowel lumen leading to hypoalbuminemia, hypogammaglobulinemia and lymphopenia [58]. Distichiasis is defined as double or more rows of eyelashes localized on the Meibomian gland orifices [59].

The YNS association with malignant disease raises the hypothesis that it might be a paraneoplastic syndrome but that notion remains controversial. The frequency of cancer being diagnosed concurrently or closely thereafter in YNS patients was estimated at 4/41 [6] and 1/21 [7]. Various types of cancers were associated with YNS: bronchial carcinoma [60, 61], breast [7, 62, 63], non-Hodgkin lymphoma [64, 65], gallbladder [6, 66], larynx [67], renal cell carcinoma [6], endometrium [68], melanoma [3], multiple myeloma after hematopoietic stem-cell transplantation [69] or precancerous mycosis fungoides [28]. The YNS-to-cancer-diagnosis interval ranges from days to years, with gradual development of the complete YNS triad [61].

YNS was occasionally associated with autoimmune diseases [70], immunodeficiency disorders, such as common variable immunodeficiency, combined T- and B-cell deficiency [70, 71], Guillain–Barré syndrome [72], nephrotic syndrome [73, 74], Hashimoto’s thyroiditis, severe hypothyroidism or hyperthyroidism [75‐77], xanthogranulomatous pyelonephritis [78] and rheumatoid arthritis even without thiol-analog use [79].

Immunological studies on YNS patients are very scarce. Isolated case reports associated YNS with IgA deficiency [22] or hypogammaglobulinemia [80]. Bokszczanin & Levinson described a 57-year-old woman with YNS and poor selective responses after vaccination against Streptococcus pneumoniae and Haemophilus influenzae [81], which might explain, in part, the recurrent lung or sinus infections in YNS. Gupta et al. reported lymphopenia in two YNS patients (one with common variable immunodeficiency) with low percentages of CD4⁺ T cells, high percentages of CD8⁺ T cells and severe naïve CD4⁺ and CD8⁺ T-cell deficits responsible for muted T-cell responses to antigens. A suggested mechanism for diminished naïve T-cell subsets might be less thymus output (thymus involution and/or apoptosis) [70]. It is of interest to note that, in another rare disease with lymphatic abnormality, primary intestinal lymphangiectasia (Waldmann’s disease), immunological investigation results were similar to those of YNS patients [82].

YNS treatment is not codified. YNS may resolve in few months without treatment [91] or, when it is a paraneoplastic syndrome, after cancer therapy [62].

Spontaneous remission of the nail changes has been observed in up to 30% of the YNS patients, regardless of treatment [5]. Remission of nail changes was more likely for fingernails than toenails, perhaps because of persistent lower limb lymphedema, which might maintain the presumed lymphatic pathophysiology [5]. More generally, the attenuated discoloration is not associated with simultaneous regression of other systemic manifestations. In YNS associated with malignant disease, treatment of the latter may lead to attenuation or disappearance of the clinical YNS signs [62, 69]. In Maldonado et al.’s study, 17 of the 37 patients with available follow-up information died after a median of 82 months [6]. In that study, a Kaplan–Meier survival curve estimated median survival at 132 months, shorter than that of a paired-control population.

YNS is very rare disorder associating yellow nail discoloration, lung manifestations/sinusitis and lymphedema. It is more frequently isolated but may be associated with other diseases implicating the lymphatic system, autoimmune diseases or cancers. Its etiology remains unknown, although lymphatic impairment is regularly evoked in the literature. Titanium is a more recent hypothetical agent but so far remains unconfirmed to explain the syndrome. YNS treatment is symptomatic for each component: yellow nails, pulmonary manifestations/sinusitis, lymphedema. Vitamin E combined with fluconazole, usually prescribed to treat yellow nails, achieves partial or complete responses. Spontaneous resolution is also possible. Research is required to better understand and treat this rare and very poorly recognized disease.