Hypopigmented Macules Research Articles

Reflectance confocal microscopy and histological features of depigmentation after local corticosteroid injection.

Clinically, depigmentation after local corticosteroid injection is not rare. But there are less articles about its reflectance confocal microscopy (RCM) and histological features. This study aimed to define the RCM features and histopathologic findings of hypopigmentation after local corticosteroid injection and to analyze the correlations between the above two methods. Forty cases with hypopigmentation after local corticosteroid injection were used to analyze the clinical and RCM features. Subsequently, for 20 of 40, an excision biopsy of the same imaged areas for histopathologic examination was executed. Our results showed that all 40 cases had round or ellipse hypopigmented macules with obscure boundary and 26 of 40 lesions' long diameter went along limbs. The RCM features and the histological findings revealed all patients had variable degrees of epidermal thinning, flattening rete ridges, reduced melanin, and no inflammatory cell infiltration. MART-1 analysisrevealed the number of melanocytes was normal but with no or less melanin by Fontana-Masson staining. Depigmentation after local corticosteroid injection was a kind of disease with intact melanocytes, whose function was impaired. RCM features offer a high consistency with histopathologic findings. It thus constitutes a promising adjuvant tool for its diagnosis and for therapeutic follow-up.

Reticulate Acropigmentation of Kitamura: A Dermoscopic Perspective.

Reticulate Acropigmentation of Kitamura: A Dermoscopic Perspective.

Tuberous Sclerosis Complex

Tuberous sclerosis complex (TSC) is an autosomal dominant inherited disorders that is characterized by the systemic hamartomas, along with epilepsy, cognitive impairment and hypopigmented macules. It is caused by genetic mutations in either TSC1 or TSC2 gene which encodes hamartin and tuberin, respectively. As the hamartin-tuberin-complex downregulates the mechanistic/mammalian target of the rapamycin complex1 (mTORC1), dysfunction in either hamartin or tuberin induces the constitutive activation of mTORC1. In fact, almost all the symptoms in TSC are derived from the activation of mTORC1. Therefore, mTORC1 inhibitors improves all the symptoms, including skin lesions and neural symptoms. Among the many symptoms, skin lesions appear earlier than renal or pulmonary lesions and are more specific than neuronal symptoms. Therefore, skin lesions are useful for the diagnosis of TSC. This chapter focuses on the features of skin lesions and mechanistic their potential role in differential diagnosis and therapy including the therapeutic use of mTORC1 inhibitors.

Speckled Acral Hypopigmentation: A New Pigmentary Disorder or an Unknown Presentation of a Known Disorder?

Sir, Reticulate pigmentary disorders are a broad group of pigmentary disorders with significant overlap, often posing a diagnostic challenge due to variable phenotypic expression of similar gene defects. The acral reticulate pigmentary disorders described so far including reticulate acropigmentation of Kitamura, Dowling–Degos disease, and acropigmentation of Dohi are characterized by the presence of hyperpigmented macules with or without hypopigmented lesions. Here, we describe a patient presenting with only hypopigmented macules in a speckled pattern on acral sites. A 17-year-old boy presented with a 2-year history of asymptomatic hypopigmented to depigmented macules on the dorsae of hands and feet. On examination, there were multiple, small (1–3mm), well-defined hypopigmented to depigmented macules symmetrically over the dorsae of hands and feet with prominent clustering over the sides. Lesions were mostly discrete, coalescing at few places, and present over a normal background skin, thus giving a speckled appearance [Figure 1a]. There were no hyperpigmented or atrophic macules, no palmar pits or break in dermatoglyphics, and no involvement of flexures. The patient was otherwise healthy with no significant medical history. He was born of nonconsanguineous marriage with no similar history in family.Figure 1: (a) Symmetric involvement of bilateral dorsae of hands and feet in form of multiple, small (1–3-mm sized), well-defined hypopigmented macules with prominent clustering over the sides. (b) Histopathology showing macromelanosomes in melanocytes as well as in keratinocytes (H and E, ×400). (c and d) Fontana-Masson and HMB-45 staining showing similar findings (×100, ×200)Two biopsies done from the hypopigmented macules of both hands showed similar features. The number of melanocytes were normal but there were a striking number of macromelanosomes in melanocytes and keratinocytes [Figure 1b]. Fontana-Masson and HMB-45 staining showed similar findings [Figure 1c and d]. Reticulate pigmentary disorders are an evolving group of dermatoses with a recent report of unusual clinical presentation as “speckled acral hypopigmentation.”The term familial was used by authors to describe a case similar to ours where a 14-year-old girl presented with speckled hypopigmentation on the sides of hands and feet bilaterally with a strong family history of similar lesions. Histopathological evaluation in this patient showed decreased number of melanocytes.[1] Congenital symmetric acroleukopathy has been described in literature, but here depigmented macules are large and present over periungual areas.[2] Reticulate acropigmentation of Kitamura is characterized by the presence of well-defined atrophic hyperpigmented macules on the dorsum of hands and feet, palmar pits, and break in dermatoglyphics.[3] Rare cases of disseminated hypo- or depigmented macules and papules are described, but presence of only hypopigmented macules is not seen in this condition.[4] Dowling–Degos disease is characterized by the presence of hyperpigmented macules over the flexures along with comedonal papules on the back and neck.[3] Rarely, Dowling–Degos disease presenting as hypopigmented macules similar to our case has been described, but in this case lesions were widely distributed over the chest, back, axilla, upper arms, and inguinal folds and there was no clustering of lesions.[5] Acropigmentation of Dohi shows presence of both hyper and hypopigmented macules on the hands and feet, which may extend to the proximal extremities and face. Extragenital lichen sclerosus is a chronic inflammatory disorder characterized by the presence of small, porcelain white, mildly atrophic polygonal papules and plaques which commonly affects neck, shoulders, and upper portion of the trunk.[6] Confetti or guttate form of hypomelanotic macules seen in tuberous sclerosis patients present as 1–3 mm, numerous, small hypopigmented macules that typically occur symmetrically over the distal extremities. These hypopigmented macules usually develop during early childhood. Over time, these patients develop other characteristic cutaneous and systemic features of tuberous sclerosis.[7] None of the above described differential diagnosis have macromelanosomes on histopathology. Histopathological differential diagnosis of macromelanosomes include Griscelli syndrome, Chediak Higashi disease, albinism, nevus spilus, neurofibromatosis, and xeroderma pigmentosum.[89] However, our patient did not have clinical features of any of the above described histopathological differentials. Our patient has an unusual clinical presentation which does not fit into any of the well described reticulate pigmentary disorders. It may be a hitherto unknown presentation of previously described disorders or it may be a unique disorder itself. Careful study of large number of patients and genomic analysis will be required to unfold this mystery. Declaration of patient consent The authors certify that they have obtained all appropriate patient consent forms. In the form the patient(s) has/have given his/her/their consent for his/her/their images and other clinical information to be reported in the journal. The patients understand that their names and initials will not be published and due efforts will be made to conceal their identity, but anonymity cannot be guaranteed. Financial support and sponsorship Nil. Conflicts of interest There are no conflicts of interest.

Sporadic Case of dyschromatosis universalis hereditaria showing moderate response to narrow-band ultraviolet-B

Dyschromatosis universalis hereditaria (DUH) is a rare genodermatosis where the affected manifests mottled pigmentation with intermingled hyper- and hypo-pigmented macules. On most occasions, the lesions begin on limbs and then extend to trunk. Most of the cases reported in literature are from Japan. It is rarer in Indians. In this report, we describe a 12-year-old male child with DUH, who showed response to narrow-band ultraviolet-B therapy.

Clinicopathological correlation in leprosy

Background: Leprosy is a chronic granulomatous disorder that is caused by Mycobacterium leprae. It mostly affects skin and peripheral nerves. The disease has varied clinical and pathological manifestations depending on the immune response of the patient. Histopathology helps in confirming the diagnosis for clinically suspicious cases and helps in exact typing which, in turn, influences treatment plan. Objectives: The objectives of this study were to study the incidence of different subtypes of leprosy and to evaluate the correlation of clinical subtype with the histopathological subtype. Materials and Methods: This was a cross-sectional comparative study done over a period of 1.5 years from August 1, 2017, to January 31, 2019, of skin biopsies of patients newly diagnosed with leprosy using routine and special stains along with clinicopathological correlation. Results: A total of 41 patients were studied between 11 and 80 years of age with a mean age of 32.64 years. Male-to-female ratio was 1.56:1. The majority of patients (41.46%) belonged to the age group of 21–30 years. Histopathologically, tuberculoid leprosy (19.51%) was the most common type followed by lepromatous leprosy and erythema nodosum leprosum (17.07% each). Clinical and histopathological concordance was seen in 65.8% of cases. The concordance was highest (100%) in histoid leprosy, indeterminate leprosy, and Type 1 lepra reaction. The most common presenting lesion was a hypopigmented macule (41.46%) followed by nodules (29.26%). Fite-Faraco positivity was 41.46%. Conclusion: Cumulative clinical, histopathological, and bacteriological diagnoses help in accurate typing of leprosy, thus facilitating appropriate therapy to prevent complications.

Late-onset amyloidosis cutis dyschromica: an unusual case

Amyloidosis cutis dyschromica (ACD) is a rare form of primary cutaneous amyloidosis. ACD, first described by Morishima in 1970 is characterized by (i) macular, speckled, reticular hyperpigmentation with hypopigmented spots distributed extensively over the body; (ii) little or no pruritus; (iii) prepubertal onset; and (iv) focal subepidermal amyloid deposition. A 49-year-old woman presented with a 20-year history of progressive, asymptomatic, generalized mottled hyper- and hypopigmented macules all over the body. Histopathological examination of a punch biopsy specimen showed deposition of homogeneous, eosinophilic material in the papillary dermis. This amorphous, eosinophilic material was stained metachromatically with crystal violet stain and found to be compatible with amyloid. Based on the clinical and histopathological findings, the patient was diagnosed as having ACD. Amyloidosis cutis dyschromica must be considered in the differential diagnosis of patients with diffuse dyschromatosis including both hyperpigmented and hypopigmented lesions and histopathological confirmation is necessary in order to reach a correct diagnosis.

Four novel mutations of ADAR1 in Chinese patients with dyschromatosis symmetrica hereditaria.

Novel mutations in adenosine deaminase acting on RNA 1 gene (ADAR1) are responsible for dyschromatosis symmetrica hereditaria (DSH). DSH patients display a mixture of hyperpigmented and hypopigmented macules on the dorsal aspects of the extremities, and freckle-like macules on the face. To provide new evidence for further study of the etiopathogenisis of DSH. Genomic DNA was extracted and used as a template for the polymerase chain reaction (PCR) amplification of all 15 coding exons as well as intron-exon boundaries of ADAR1. The PCR products were sequenced directly. We identified eight mutations of ADAR1 in four Chinese pedigrees and four individual patients, which were c.2722G>T, p.(Asp908Tyr), c.1657delA, p.(Ser553fs), c.2563_2564delCT, p.(Leu855fs), c.526T>G, p.(Leu176Val) as well as four previously reported mutations c. 3363_3364insT, p.(Lys1122fs), c. 2865_2866delGT, p.(Val955fs), c.1630C>T, p.(Arg544X), and c.2894C>T, p.(Pro965Leu). In silico analysis predicted that all the mutations reported were pathogenic. We did not study how ADAR1 played its role in DSH. So, the exact pathogenic mechanism of ADAR1 in DSH patients wasn't clarified in this study. We found four novel ADAR1 mutations in this study. Our results enlarge the database on ADAR1 mutations associated with DSH.

Dermoscopy is a new diagnostic tool in diagnosis of common hypopigmented macular disease: A descriptive study.

One of the most frequent complaints in dermatology clinics is the eruption of hypopigmented patchy skin lesions. The aim of the study was to investigate the utility of dermoscopy in common hypopigmented macular diseases. Patients with the followings diseases were examined by dermoscopy: vitiligo, pityriasis alba, nevus depigmentosus, achromic pityriasis versicolor, idiopathic guttate hypomelanosis, and extragenital guttate lichen sclerosus.This study showed that these hypopigmented macular diseases might display specific dermoscopic features. In vitiligo, the mean dermoscopic features were the presence of a diffuse white glow with perifollicular pigment, perilesional hyperpigmentation, leukotrichia and the pigmentary network. In idiopathic guttate hypomelanosis, the characteristic features were the presence of multiple, shiny, scaly macules with welland ill-defined edges borders that coalesced into polycyclic macules. For nevus depigmentosus, the mean features were hypopigmented patches with irregular border with a faint reticular network. For pityriasis alba, the fairly ill-demarcated hypopigmented macules with fine scales were the mean feature. In lichen sclerosus, there were white structureless areas, perilesional erythematous halo, follicular plugging and white chrysalis like structures. Dermoscopy of achromic pityriasis versicolor showed a fairly demarcated white area with fine scales localized in the skin creases.

自身免疫性多腺体综合征IV型：胸腺瘤、白癜风、重症肌无力、系统性红斑狼疮、寻常型天疱疮及普秃并发一例

On November 30th, 2017, a 62-year-old female patient was admitted to the hospital because of multiple depigmented patches all over the body for 16 years, as well as erythema and blisters on the scalp, trunk and upper extremities for more than 8 years, which had been aggravated for 1 year. The patient underwent surgical resection of thymoma in 1996, and developed myasthenia gravis in 2004. Skin examination showed scattered erythemas of various sizes on the scalp, face, chest and upper extremities, with crusts on the surface of some erythemas and positive Nikolsky′s sign. Hypopigmented macules mingled with depigmentated macules of various sizes were scattered all over the body. A large area of depigmentation was observed on both hands, and the nail plates were atrophic. Hairs, eyebrows, eyelashes, axillary and pubic hairs were abscent. Laboratory examination showed the presence of homogeneous IgG antinuclear antibody with a titer of 1∶640, anti-double stranded DNA antibody (276 IU/ml) , lupus anticoagulant (1.62) , anti-Dsg1 antibody (> 150 U/ml) and anti-Dsg3 antibody (91 U/ml) . Histopathological examination of dorsal blister tissues and hematoxylin-eosin staining showed fissured blisters and acantholytic cells in the epidermis, monolayer basal cells on the basilar membrane, and perivascular infiltration of a few lymphocytes in the superficial dermis. The patient successively developed thymoma, vitiligo, myasthenia gravis, systemic lupus erythematosus, pemphigus vulgaris and alopecia universalis, so a diagnosis of autoimmune polyglandular syndrome type Ⅳ was made. Since autoimmune-mediated endocrinopathies are prone to occur successively, changes of related hormones and antibodies in the patient should be monitored for early diagnosis and treatment of newly emerging autoimmune diseases. Key words: Thymoma; Vitiligo; Pemphigus; Myasthenia gravis; Lupus erythematosus, systemic; Alopecia; Autoimmune polyglandular syndrome

Multiple hypochromic or achromic macules in children and risk of tuberous sclerosis

To describe in a large paediatric cohort the characteristics of hypopigmented and depigmented (hypochromatic and achromic) macules with no clear diagnosis but potentially evocative of tuberous sclerosis (TS). This was a retrospective multicentre study performed between 2010 and 2017 at a reference centre for rare skin diseases; it included all children consulting for hypochromic and achromic macules. A descriptive analysis was made of the characteristics of macules with no clear diagnosis, enabling them to be classified in three secondary groups: TS certain, TS ruled out, TS uncertain. Of the 3300 children seen during this 7-year period 7,265 were consulting for hypochromic or achromic macules, with no clear diagnosis in 18 cases: 7 girls and 11 boys of median age at 7.21 years (range: 4 months to 16 years and 7 months). The lesions were congenital in 7 cases. The number of macules varied, with over 20 in some cases. The majority were in the form of ash-leaf spots, followed by the oval form. Two children were diagnosed at clinical examination, and 16 underwent it is not examinations, resulting in a diagnosis of certain ST in 6 of these cases. No particular characteristics of the macules appeared to guide the clinical examination towards ST or isolated lesions. Café-au-lait spots were more frequent in the group in which ST was ruled out than in the other two groups: 67% vs. 33% and 33%. Neurologic involvement was more common in children with certain or uncertain ST than in children in whom ST was ruled out (83% and 67% vs. 11%). No identified characteristics of stains enabled the clinical examination to confirm or rule out tuberous sclerosis. Screening for acute any signs of ST is essential. Diagnostic efficacy is enhanced by additional exams.

Atypical tuberous sclerosis complex presenting as familial renal cell carcinoma with leiomyomatous stroma

We report an atypical tuberous sclerosis complex (TSC) phenotype presenting as familial multiple renal cell carcinomas (RCCs) with (angio)leiomyomatous stroma (RCCLS) (5/7 familial RCCs) on a background of multiple angiomyolipomas, hypopigmented skin macules, and absence of neurological anomalies. In the index case and three relatives, germline genetic testing identified a heterozygous TSC2 missense pathogenic variant [c.2714 G > A, (p.Arg905Gln)], a rare TSC‐associated alteration which has previously been associated with a milder TSC phenotype. Whole‐exome sequencing of five RCCs from the index case and one RCC from his mother demonstrated either unique tumour‐specific deleterious second hits in TSC2 or significant allelic imbalance at the TSC2 gene locus (5/6 RCCs). This study confirms the key tumourigenic role of tumour‐specific TSC2 second hits in TSC‐associated RCCs and supports the notion that RCCLS may be strongly related to abnormalities of the mTOR pathway.

Dyskeratosis congenita with a novel genetic variant in the DKC1 gene: a case report

BackgroundDyskeratosis congenita (DC) is a rare genetic disorder of bone marrow failure inherited in an X-linked, autosomal dominant or autosomal recessive pattern. It has a wide array of clinical features and patients may be cared for by many medical sub specialties. The typical clinical features consist of lacy reticular skin pigmentation, nail dystrophy and oral leukoplakia. As the disease advances, patients may develop progressive bone marrow failure, pulmonary fibrosis, oesophageal stenosis, urethral stenosis, liver cirrhosis as well as haematological and solid malignancies. Several genes have been implicated in the pathogenesis of dyskeratosis congenita, with the dyskerin pseudouridine synthase 1 (DKC1) gene mutations being the X-linked recessive gene.Case presentationHerein, we report a 31-year-old male with history of recurrent febrile episodes who was found to have reticulate skin pigmentation interspersed with hypopigmented macules involving the face, neck and extremities, hyperkeratosis of palms and soles, nail dystrophy, leukoplakia of the tongue, premature graying of hair, watery eyes and dental caries. Several of his male relatives, including two maternal uncles and three maternal cousins were affected with a similar type of disease condition. Pedigree analysis suggested a possible X-linked pattern of inheritance. Genetic testing in the proband showed a novel hemizygous, non-synonymous likely pathogenic variant [NM_001363.4: c.1054A > G: p.Thr352Ala] in the PUA domain of the DKC1 gene. Quantitative polymerase chain reaction for relative telomere length measurements performed in the proband showed that he had very short telomeres [0.38, compared to a control median of 0.71 (range 0.44–1.19)], which is consistent with the DC diagnosis. Co-segregation analysis of the novel mutation and telomere length measurements in the extended family members could not be performed as they were unwilling to provide consent for testing.ConclusionsThe novel variant detected in the DKC1 gene adds further to the existing scientific literature on the genotype-phenotype correlation of DC, and has important implications for the clinical and molecular characterization of the disease.

Clinical and histological profile of leprosy patients at rural based tertiary care centre in post elimination era

Background: Despite India having achieved the national leprosy elimination goal of prevalence rate less than one case per 10000, the disease is still prevalent. Its diverse presentation depending on immune status of host warrants a clinico-histological correlation for diagnosis and start of proper therapy.Aim: The present study was done with the aim to describe the spectrum of clinical and histological profile of leprosy patients especially in doubtful and difficult cases especially where the clinical diagnosis is not sufficient and, then, to correlate clinical and histological profile.Methods: This study is a hospital based prospective study conducted on sixty newly diagnosed cases of leprosy. Skin biopsy was taken in each case and processed routinely. All the cases were stained with hematoxylin and eosin and modified Ziehl-Neelsen stain. Ridley-Jopling classification was used for diagnosis and typing of cases.Results: In the present study consisting of 60 newly diagnosed leprosy patients, majority of the cases i.e. 18 (30%) were in age group of 21-30 years with male: female ratio of 1.6:1. The most common type of skin lesion was plaque (50%), followed by hypo-pigmented macule (33.3%). The clinico-pathological concordance was maximum in Tuberculoid (TT) (100%) followed by Lepromatous (LL) (80%), Borderline lepromatous (BL) (72.7%), Borderline tuberculoid (BT) (50%) and Mid-borderline (BB) (33.3%).Conclusion: The overall clinicopathological concordance in present study is good (66.7%). Thus, the correlation of clinical and histological features along with bacillary index is far more useful for accurate typing and therapy in leprosy patients.DOI:10.21276/APALM.1680

Multisystem Langerhans cell histiocytosis in an infant: A case report and review of literature

Langerhans cell histiocytosis (LCH) is a rare disease of childhood which originates from marrow-derived immature myeloid dendritic cells of skin and visceral organs with incompletely understood etiopathogenesis. An 11-month-old infant presented with fever, pallor, multiple erythematous, crusted, scaly hypopigmented macules, and shiny colored papules over scalp, forehead, and trunk along with hepatosplenomegaly. Persistent pancytopenia, punched out lesion on a brain scan, and multinucleated giant cells with eosinophilic cytoplasm admixture with eosinophils and lymphocytes on skin biopsy were seen. Immunohistochemistry was positive for CD1a and S100. The patient was treated with vinblastine and steroid, but unfortunately parents did not complete the therapy. A high index of suspicion is necessary to make timely diagnosis and therapy to minimize the frustration felt by parents/patients.

Pityriasis versicolor in children: a study of 110 cases

<p class="abstract"><strong>Background:</strong> <span lang="EN-GB">Pityriasis versicolor (PV) is a cutaneous fungal infection caused by the yeast fungus <em>Malassezia</em>. Though common in adults, children can also develop PV</span><span lang="EN-IN">.</span></p><p class="abstract"><strong>Methods:</strong> <span lang="EN-GB">110 cases of clinically and mycologically proven cases of PV in children upto 14 years were included in this study which was conducted in the Dermatology outpatient department of Karuna Medical College, Palakkad over a period of one year</span>.<strong></strong></p><p class="abstract"><strong>Results:</strong> <span lang="EN-GB">PV in children accounted for 22.63% of total cases of PV seen during the study period. Face was the commonest site involved (78%). Majority (83.64%) presented with hypopigmentation and family history was present in 26%. Most cases (67%) were seen during the months of April to September</span><span lang="EN-IN">. </span></p><p class="abstract"><strong>Conclusions:</strong> <span lang="EN-GB">PV in children is not rare and it commonly presents as asymptomatic hypopigmented macules over the face</span><span lang="EN-IN">.</span></p>

Loss of GPNMB Causes Autosomal-Recessive Amyloidosis Cutis Dyschromica in Humans

Amyloidosis cutis dyschromica (ACD) is a distinct form of primary cutaneous amyloidosis characterized by generalized hyperpigmentation mottled with small hypopigmented macules on the trunks and limbs. Affected families and sporadic case subjects have been reported predominantly in East and Southeast Asian ethnicities; however, the genetic cause has not been elucidated. We report here that the compound heterozygosity or homozygosity of GPNMB truncating alleles is the cause of autosomal-recessive ACD. Six nonsense or frameshift mutations were identified in nine individuals diagnosed with ACD. Immunofluorescence analysis of skin biopsies showed that GPNMB is expressed in all epidermal cells, with the highest staining observed in melanocytes. GPNMB staining is significantly reduced in the lesional skin of affected individuals. Hyperpigmented lesions exhibited significantly increased amounts of DNA/keratin-positive amyloid deposits in the papillary dermis and infiltrating macrophages compared with hypo- or depigmented macules. Depigmentation of the lesions was attributable to loss of melanocytes. Intracytoplasmic fibrillary aggregates were observed in keratinocytes scattered in the lesional epidermis. Thus, our analysis indicates that loss of GPNMB, which has been implicated in melanosome formation, autophagy, phagocytosis, tissue repair, and negative regulation of inflammation, underlies autosomal-recessive ACD and provides insights into the etiology of amyloidosis and pigment dyschromia.

The Disturbance of Melanogenesis and Melanosome Transfer in the Leukoderma Lesions of Extramammary Paget’s Disease

We frequently encounter characteristic color variation including hypopigmentation, hyperpigmentation, and erythema in extramammary Paget’s disease (EMPD) lesions. Owing to unclear hypopigmentation, the lesional border of EMPD can be poorly defined and it is likely insufficient to perform its complete resection. Although the existence of Toker’s cells and lack of lesional bFGF production have been reported to cause hypopigmentation inside of EMPD lesions, exact mechanisms of hypopigmentation in EMPD are not fully explored. We experienced three EMPD patients with obviously hypopigmented EMPD macules and histopathologically confirmed a reduced number of melanocytes on the hypopigmented macules and their loss on the erythematous plaques or nodules. An ultrastructural analysis on the hypopigmented lesions revealed disturbance of melanosome maturation and melanosome transfer to the adherent Pagets’ cell on the basal layer. No Paget’s cells even adhered to remaining melanocytes with dendrites contained matured melanosome and a few number of matured melanosome complexes were observed in basal keratinocytes. In the present study, we hypothesize that severe disturbance of not only melanogenesis but also melanosome transfer to surrounding Paget’s cells and basal keratinocytes may cause characteristic hypopigmentation in EMPD. Future bioanalysis would reveal molecular mechanisms for hypopigmentation in EMPD.

A Case of Punctate Leukoderma after 1,064 nm Q-Switched Nd:YAG Laser

Punctate leukoderma is characterized of the destruction of melanocytes after chemical of physical damage. In addition, the term is broadly used to describe hypopigmented lesions induced in vitiligo patients after psolaren administration with ultraviolet A and in psoriasis patients with repetitive ultraviolet B phototherapy. The Q-switched neodymium-doped yttrium aluminum garnet (Nd:YAG) laser in treating melasma is frequently reported to be associated with the cause. A 44-year-old woman presented to the department with numerous confetti-like hypopigmented macules on both cheeks for over a year. Weekly treatment of 1,064 nm Q-switched Nd:YAG laser (2.0–3.4 J, 8 mm spot-size) therapy at a non-dermatologic clinic had induced both hyperpigmentation and hypopigmentation lesions. Biopsy performed at both hyperpigmented and hypopigmented lesions revealed variable melanin pigmentation with segmental loss and infiltration of pigment incontinence. The patient was diagnosed with punctate leukoderma and was directed for narrow-band ultraviolet B phototherapy. Herein, we report a case of punctate leukoderma after inadvertent use of 1,064 nm Q-switched Nd:YAG laser. Key words: Masson-Fontana; Punctate leukoderma; Q-switched Nd:YAG

Notalgia paresthetica: a review for dermatologists.

Notalgia paresthetica (NP) is an underdiagnosed condition that presents with unilateral pruritus medial to the scapula on the midback with or without an associated hyperpigmented or hypopigmented macule. There is a paucity of recent reviews on this chronic cutaneous neuropathy in peer-reviewed journals. Current theories propose the condition is likely multifactorial, including spinal entrapment and muscular compressive neuropathy. An extensive literature review was performed by searching the MEDLINE database to review all published works on notalgia paresthetica. This review will provide a useful update for clinicians on the pathogenesis, clinical features, biopsy features, risk factors, and management options for this condition including pharmacological and nonpharmacological methods detailing published treatment options to date for this difficult to treat condition.