Revive the Dennie-Morgan Fold: A Forgotten Sign of Atopic Dermatitis in Children.

Rohan Shah, William C Lambert, Robert A Schwartz
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Abstract

In 1980, Hanifin and Rajka (1) proposed major and minor diagnostic criteria for atopic dermatitis (AD). Major associations included pruritus, dry skin, and history of atopy. One minor feature included Dennie-Morgan Folds (DMFs), which manifest as secondary creases in the skin underneath the inferior eyelid, usually found in infants (2). In an attempt to refine these criteria, a study evaluating 210 patients with an existing AD diagnosis observed DMF in 84% of AD cases. A pediatric study in Bijapur, India on 174 children under 16 years of age with AD identified DMF to be the most prevalent minor criterion. DMFs were found in 71.8% of the study's population and was followed by palmar hyperlinearity and xerosis in prevalence (2). Although DMF pathophysiology remains unclear, we suggest a theory stemming from nocturnal pruritus (NP). The two leading causes of NP are AD and psoriasis, both of which interfere with the patient's sleep quality. Children with increased NP have greater sleep fragmentation and difficulty waking up in the morning (3). A lack of melatonin rhythmic secretions resulting in circadian misalignment may serve as an intermediary for DMF onset. As more blood perfuses the skin under the eyes, edematous fluid enhances dysregulation of the collagen fibers under the eyelids. NP also manifests as facial touching and rubbing or scratching the eyelids during sleep, which can aggravate tissue surrounding the eye (3). AD affects 15-20% of the pediatric population, whereas food allergies, some life-threatening, are found in up to 30% of children with AD, compared with 0.1-0.6% of children in the general population (2). Identifying DMF in children can facilitate the diagnosis of AD and thus lead to the necessary tests to determine whether conditions associated with AD exist, such as food allergy. DMFs are indicative of an AD diagnosis and can be especially critical for children who have life-threatening food allergies associated with their AD (3). One challenge in using DMF as a marker for AD are its different manifestations across ethnic and racial groups. In a study of 160 children aged 3-11 years in London, England, DMFs were present in 34/69 children classified as "black", regardless of whether the child presented with AD. In children classified as "white", only 11/44 had DMFs regardless of AD diagnosis. When cases of AD were excluded, 25% of the white children and 49% of black children had DMFs (4). In a separate study evaluating the differences in prevalence of AD minor characteristics between African Americans and European Americans, African Americans were more likely to have extensor involvement along with diffuse xerosis, palmar hyperlinearity, and DMFs (5). Furthermore, in individuals with darker skin tones, DMFs may be of greater importance, as other characteristics such as erythema may be harder to recognize (5). Life-threatening food allergies are rare, but represent serious sequelae associated with AD. DMFs can serve as a critically simple, easy-to-identify marker for AD and perhaps identify the condition before the presence of serious sequelae. DMFs may guide the clinician towards inquiring further about other AD-related symptoms, thus improving clinical assessment of a significant pediatric condition.

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重现丹尼-摩根皱褶:被遗忘的儿童特应性皮炎体征
1980 年,Hanifin 和 Rajka(1)提出了特应性皮炎(AD)的主要和次要诊断标准。主要特征包括瘙痒、皮肤干燥和过敏史。一个次要特征包括 Dennie-Morgan 皱褶(DMFs),表现为下眼睑下方皮肤的继发性皱褶,通常出现在婴儿身上(2)。为了完善这些标准,一项对 210 名已确诊为注意力缺失症的患者进行评估的研究发现,84% 的注意力缺失症病例存在 DMF。印度比贾布尔的一项儿科研究对174名16岁以下的AD患儿进行了调查,结果发现DMF是最常见的次要标准。研究发现,71.8%的研究对象存在DMF,其次是掌纹过长和干燥症(2)。尽管 DMF 的病理生理学尚不清楚,但我们提出了一种源自夜间瘙痒(NP)的理论。引起夜间瘙痒的两个主要原因是注意力缺失症和银屑病,这两种疾病都会影响患者的睡眠质量。夜间瘙痒症加重的儿童睡眠碎片更多,早晨起床困难(3)。缺乏褪黑激素节律性分泌导致昼夜节律失调可能是 DMF 发病的中间因素。由于更多的血液灌注到眼下的皮肤,水肿的液体加剧了眼睑下胶原纤维的失调。NP还表现为面部触摸、睡眠时揉搓或抓挠眼睑,这会使眼睛周围的组织恶化(3)。15%-20%的儿童患有注意力缺失症,而高达30%的注意力缺失症患儿对食物过敏,其中有些会危及生命,而普通人群中对食物过敏的儿童仅占0.1%-0.6% (2)。识别儿童 DMF 有助于 AD 的诊断,从而进行必要的检查以确定是否存在与 AD 相关的疾病,如食物过敏。DMF 是 AD 诊断的指示性指标,对于那些因食物过敏而导致 AD 并危及生命的儿童尤为重要 (3)。将DMF作为AD的标志物所面临的一个挑战是,不同民族和种族群体的DMF表现各不相同。在一项针对英国伦敦 160 名 3-11 岁儿童的研究中,34/69 名被归类为 "黑人 "的儿童出现了 DMF,无论他们是否出现 AD。在被归类为 "白人 "的儿童中,无论是否诊断出注意力缺失症,只有11/44的儿童有DMFs。如果排除注意力缺失症病例,25%的白人儿童和49%的黑人儿童有DMFs(4)。另一项研究评估了非裔美国人和欧裔美国人在注意力缺失症次要特征患病率上的差异,结果显示,非裔美国人更有可能出现伸肌受累、弥漫性角化病、掌纹过度线性和 DMFs(5)。此外,对于肤色较深的人来说,DMFs 可能更为重要,因为红斑等其他特征可能更难识别(5)。危及生命的食物过敏并不多见,但却代表着与 AD 相关的严重后遗症。DMF 可以作为 AD 的一个非常简单、易于识别的标记,或许可以在出现严重后遗症之前识别出病情。DMFs可以指导临床医生进一步询问其他与AD相关的症状,从而改善对重要儿科疾病的临床评估。
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