Magdalene A Dohil’s research while affiliated with Rady Children's Hospital and other places

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Publications (34)


Skin biopsies and intradermal confocal imaging highlight crystals in cystinosis patients
A-C, Skin punch biopsies taken from 1–2 cm behind the mastoid region of the right ear of two cystinosis patients (A-B) and a healthy control (C). Skin biopsy samples were sectioned at 1 μm and then stained with Toluidine Blue to detect cystine crystals and H&E for structural evaluation. Arrows indicate crystals. Crystal counting and morphological measurements were conducted by a clinical pathologist. Scale bar toluidine blue = 50 μm. Scale bar H&E = 100 μm. White arrowhead indicate perivascular chronic inflammatory cells in the upper dermis (A). L = lymphocyte, F = fibroblast nucleus, Sq. Epi. = squamous cell epithelium, BV = blood vessel. D, Intradermal imaging methodology and sample patient image. Using a handheld RCM device, a 78 slice Zstack with step size of 2.8 μm was taken behind the left ear beginning within the epidermis. A representative single slice with arrows indicating crystals is shown, while complete patient and control Zstacks are provided in S1 and S2 Videos. Scale bar = 100 μm.
Automated 2D and 3D image analysis detects an increased crystallization in cystinotic skin
A total of 83 image stacks were acquired from 70 cystinosis patients and 38 from 27 healthy controls. A, Workflow from initial selection of total crystals and skin structure to final 3D reconstruction of the papillary dermis region. Arrows indicate false-positive crystals which are eliminated due to overlap with skin structure. Full description of methodology may be found in S1 Fig and Supplementary Methods in (S1 File). B, Representative slices from raw and 2D analyzed intradermal confocal micrographs from a healthy control and patients. XY scatterplot displays the sum of crystal area normalized to total imaged region on the Y-axis vs. tissue depth on X-axis. Arrows indicate which slice is the sample image. C, XY scatterplot depicting mean crystal area +/- SD vs. tissue depth for grouped cystinosis patients vs. healthy controls. For subjects with multiple images, only the most recent encounter was included. Starred region indicates slices where patients have significantly higher crystal area. D, 3D reconstructions of healthy and patient crystal density exclusively in the papillary dermal region due to signal background in epidermis and hypodermis; see Results section “Crystal quantification by automated image analysis in 2D” for details. Representative videos are provided in S3 and S4 Videos. E, Boxplot comparing sum crystal volume in papillary dermis (nCCV) +/- SD between patients and controls. **** = P<0.001. All scale bars = 100 μm.
Focused case study investigating predictive potential of nCCV for two cystinosis patients
A-B, Intradermal imaging and analysis in 2D and 3D for two cystinosis subjects: Subject 1, a 20 yr-old compliant male without a kidney transplant and compound heterozygous for the 57kb deletion and a frameshift mutation (A), and Subject 2, a 31 yr-old non-compliant patient, bearing the 57kb deletion in the homozygous state, who has received his first kidney transplantation at 14 years and second at 26 years of age (B). Scale bar = 100 μm. C, nCCV quantitation of Patients 1 and 2 for multiple years of acquisition. (D) Selected medical outcomes displaying subject 1 (blue star) and subject 2 (red star) compared to the full set of patients (each dot represents a patient) for various symptoms during the most recent year of acquisition, n = 36 for TSH, n = 31 for PTH, n = 41 for BP Systolic, and n = 37 for BMI.
Demographic and clinical characteristics of infantile cystinosis patients
Association between nCCV and various medical outcomes
Non-invasive intradermal imaging of cystine crystals in cystinosis
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March 2021

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155 Reads

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4 Citations

Marya Bengali

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Xiaoying Sun

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Importance Development of noninvasive methodology to reproducibly measure tissue cystine crystal load to assess disease status and guide clinical care in cystinosis, an inherited lysosomal storage disorder characterized by widespread cystine crystal accumulation. Objective To develop an unbiased and semi-automated imaging methodology to quantify dermal cystine crystal accumulation in patients to correlate with disease status. Design, setting and participants 101 participants, 70 patients and 31 healthy controls, were enrolled at the University of California, San Diego, Cystinosis Clinics, Rady Children’s Hospital, San Diego and at the annual Cystinosis Research Foundation family conference for an ongoing prospective longitudinal cohort study of cystinosis patients with potential yearly follow-up. Exposures Intradermal reflectance confocal microscopy (RCM) imaging, blood collection via standard venipuncture, medical record collection, and occasional skin punch biopsies. Main outcomes and measures The primary outcome was to establish an automated measure of normalized confocal crystal volume (nCCV) for each subject. Secondary analysis examined the association of nCCV with various clinical indicators to assess nCCV’s possible predictive potential. Results Over 2 years, 57 patients diagnosed with cystinosis (median [range] age: 15.1 yrs [0.8, 54]; 41.4% female) were intradermally assessed by RCM to produce 84 image stacks. 27 healthy individuals (38.7 yrs [10, 85]; 53.1% female) were also imaged providing 37 control image stacks. Automated 2D crystal area quantification revealed that patients had significantly elevated crystal accumulation within the superficial dermis. 3D volumetric analysis of this region was significantly higher in patients compared to healthy controls (mean [SD]: 1934.0 μm³ [1169.1] for patients vs. 363.1 μm³ [194.3] for controls, P<0.001). Medical outcome data was collected from 43 patients with infantile cystinosis (media [range] age: 11 yrs [0.8, 54]; 51% female). nCCV was positively associated with hypothyroidism (OR = 19.68, 95% CI: [1.60, 242.46], P = 0.02) and stage of chronic kidney disease (slope estimate = 0.53, 95%CI: [0.05, 1.00], P = 0.03). Conclusions and relevance This study used non-invasive RCM imaging to develop an intradermal cystine crystal quantification method. Results showed that cystinosis patients had increased nCCV compared to healthy controls. Level of patient nCCV correlated with several clinical outcomes suggesting nCCV may be used as a potential new biomarker for cystinosis to monitor long-term disease control and medication compliance.

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Idiopathic facial aseptic granuloma—A diagnostic challenge in pediatric dermatology

February 2018

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60 Reads

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17 Citations

Pediatric Dermatology

Idiopathic facial aseptic granuloma is a distinct, benign lesion that presents in very young children and is characterized by a painless facial nodule that usually appears on the cheek. It is typically characterized by a prolonged course but heals spontaneously or in response to antibiotic treatment. The challenge is to diagnose this entity correctly, ideally based on clinical acumen, to avoid surgical intervention with facial sutures and the resultant scarring and unnecessary treatment interventions. In this article, we discuss three cases of idiopathic facial aseptic granuloma to raise awareness and highlight the diagnostic challenges and possible link to childhood rosacea.



The Harmonising Outcome Measures for Eczema (HOME) statement to assess clinical signs of atopic eczema in trials

October 2014

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195 Reads

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299 Citations

Journal of Allergy and Clinical Immunology

The lack of core outcome sets for atopic eczema (AE) is a major obstacle for advancing evidence-based treatment. The global Harmonising Outcome Measures for Eczema (HOME) initiative has already defined clinical signs, symptoms, quality of life, and long-term control of flares as core outcome domains for AE trials. This article deals with the standardization of measurement instruments to assess clinical signs of AE. To resolve the current lack of standardization of the assessment of clinical signs of AE, we followed a structured process of systematic reviews and international consensus sessions to identify 1 core outcome measurement instrument for assessment of clinical signs in all future AE trials. Systematic reviews indicated that from 16 different instruments identified to assess clinical signs of AE, only the Eczema Area and Severity Index (EASI) and the objective Scoring Atopic Dermatitis (SCORAD) index were identified as extensively validated. The EASI has adequate validity, responsiveness, internal consistency, and intraobserver reliability. The objective SCORAD index has adequate validity, responsiveness, and interobserver reliability but unclear intraobserver reliability to measure clinical signs of AE. In an international consensus study, patients, physicians, nurses, methodologists, and pharmaceutical industry representatives agreed that the EASI is the preferred core instrument to measure clinical signs in all future AE trials. All stakeholders involved in designing, reporting, and using clinical trials on AE are asked to comply with this consensus to enable better evidence-based decision making, clearer scientific communication, and improved patient care.


Figure 1: Breakdown of meeting participants by stakeholder group.
Figure 2. The Harmonizing Outcome Measures for Eczema (HOME) roadmap to develop core sets of outcome measurement instruments. *For trials the scope should generally be global.
Report from the Third International Consensus Meeting to Harmonise Core Outcome Measures for Atopic Eczema / Dermatitis Clinical Trials (HOME).

July 2014

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249 Reads

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107 Citations

British Journal of Dermatology

This report provides a summary of the third meeting of the Harmonising Outcome Measures for Eczema (HOME) initiative held in San Diego, CA, U.S.A., 6–7 April 2013 (HOME III). The meeting addressed the four domains that had previously been agreed should be measured in every eczema clinical trial: clinical signs, patient-reported symptoms, long-term control and quality of life. Formal presentations and nominal group techniques were used at this working meeting, attended by 56 voting participants (31 of whom were dermatologists). Significant progress was made on the domain of clinical signs. Without reference to any named scales, it was agreed that the intensity and extent of erythema, excoriation, oedema/papulation and lichenification should be included in the core outcome measure for the scale to have content validity. The group then discussed a systematic review of all scales measuring the clinical signs of eczema and their measurement properties, followed by a consensus vote on which scale to recommend for inclusion in the core outcome set. Research into the remaining three domains was presented, followed by discussions. The symptoms group and quality of life groups need to systematically identify all available tools and rate the quality of the tools. A definition of long-term control is needed before progress can be made towards recommending a core outcome measure.



Natural Ingredients in Atopic Dermatitis and Other Inflammatory Skin Disease

September 2013

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356 Reads

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10 Citations

Journal of Drugs in Dermatology

Active naturals in dermatology have been experiencing a renaissance. Many of the naturals that have been known for centuries to be effective for various skin conditions have now been scientifically validated with the unraveling of the pathophysiology behind their medicinal mechanism. This article seeks to present data on the clinical use of key dermatological active naturals such as oatmeal, feverfew, chamomile, aloe vera, licorice, and dexpanthenol, as well as on recent multicenter and international clinical studies that support their efficacy and safety profile for a variety of inflammatory skin conditions. J Drugs Dermatol. 2013;12(suppl 9):s128-s132.


Towards global consensus on outcome measures for atopic eczema research: Results of the HOME II meeting

July 2012

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127 Reads

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175 Citations

The use of nonstandardized and inadequately validated outcome measures in atopic eczema trials is a major obstacle to practising evidence-based dermatology. The Harmonising Outcome Measures for Eczema (HOME) initiative is an international multiprofessional group dedicated to atopic eczema outcomes research. In June 2011, the HOME initiative conducted a consensus study involving 43 individuals from 10 countries, representing different stakeholders (patients, clinicians, methodologists, pharmaceutical industry) to determine core outcome domains for atopic eczema trials, to define quality criteria for atopic eczema outcome measures and to prioritize topics for atopic eczema outcomes research. Delegates were given evidence-based information, followed by structured group discussion and anonymous consensus voting. Consensus was achieved to include clinical signs, symptoms, long-term control of flares and quality of life into the core set of outcome domains for atopic eczema trials. The HOME initiative strongly recommends including and reporting these core outcome domains as primary or secondary endpoints in all future atopic eczema trials. Measures of these core outcome domains need to be valid, sensitive to change and feasible. Prioritized topics of the HOME initiative are the identification/development of the most appropriate instruments for the four core outcome domains. HOME is open to anyone with an interest in atopic eczema outcomes research.


Citations (26)


... Reflectance confocal microscopy allows differentiation of the density, within skin, of crystal-containing particles that are present in higher quantities in older patients and in those who started cysteamine treatment later [55]. This method, coupled with an automated and unbiased imaging tool for the quantification of crystal area and volume, makes cystine crystals in skin a novel biomarker that can facilitate long-term monitoring of cystinosis patients in clinical practice [70]. The study by Bengali et al. [70] expanded the observation of Chiaverini et al. [55], monitoring 70 cystinosis patients for over two years through analysis of punch skin biopsy and the quantification of images of 2D area and 3D volume of crystals in dermis, compared to 27 healthy controls. ...

Reference:

Biomarkers in Nephropathic Cystinosis: Current and Future Perspectives
Non-invasive intradermal imaging of cystine crystals in cystinosis

... The histopathological findings can vary based on the clinical presentation of childhood rosacea, but dense dermal granulomatous inflammation in the perifollicular area is a common feature, similar to the cutaneous form of childhood rosacea [8]. Dermoscopy, a noninvasive tool initially used for skin tumors, is also effective in diagnosing the telangiectatic subtype of childhood rosacea, revealing a unique pattern of linear and polygonal vessels [30]. In adults with rosacea, especially the erythematotelangiectatic type, dermoscopy reveals vascular abnormalities such as polygonal and branched vessels. ...

Idiopathic facial aseptic granuloma—A diagnostic challenge in pediatric dermatology
  • Citing Article
  • February 2018

Pediatric Dermatology

... 33 Other excipients included to aid in reducing the potential for skin irritation and also reported to exhibit antiinflammatory effects are allantoin, panthenol, and glycerretinic acid. 44,45 Silica microbeads and corn starch are included as sebum absorbants adaptable for patients with oily skin to reduce "facial shine" and skin oiliness/greasiness, but are not problematic for patients with normal or dry skin. 33,41 A matte-effect powder is also included to produce a smooth, non-shiny overall appearance to facial skin. ...

Atopic Dermatitis and Other Inflammatory Skin Disease - Natural Ingredients for Skin Care and Treatment
  • Citing Article
  • September 2011

Journal of Drugs in Dermatology

... The Eczema Area and Severity Index (EASI) measure was recommended as a core outcome by the Harmonizing Outcome Measures for Eczema (HOME) international consensus group to assess clinical signs of AD (12). An EASI 75 response (75% improvement in EASI) is commonly used as a primary endpoint or co-primary endpoint along with the Investigator Global Assessment (IGA) to assess AD treatment efficacy in clinical trials (13). ...

The Harmonising Outcome Measures for Eczema (HOME) statement to assess clinical signs of atopic eczema in trials
  • Citing Article
  • October 2014

Journal of Allergy and Clinical Immunology

... The LIBERTY AD PRESCHOOL part B study, a phase 3 placebo-controlled trial in children aged 6 months to 5 years with moderatetosevere AD, showed significant improvements in AD signs, symptoms, and QoL in children receiving dupilumab with concomitant low-potency topical corticosteroids (TCS). As required by regulatory authorities, the primary endpoint in that trial was achievement of an Investigator's Global Assessment (IGA) score of 0 or 1 (clear or almost clear skin) (12,14,15). Although IGA is widely used because of its simplicity and convenience in the assessment of skin signs, it does not take into account the multidimensional aspects of AD impacting the patient's QoL, including symptoms such as itch, and the body surface area (BSA) affected by AD lesions. ...

Report from the Third International Consensus Meeting to Harmonise Core Outcome Measures for Atopic Eczema / Dermatitis Clinical Trials (HOME).

British Journal of Dermatology

... A few archetypes of KHE/TA have emerged and may help guide initial treatment decisions and clinical trial design: (1) fulminant KHE with KMP in a neonate/young infant, (2) large cutaneous/noncutaneous KHE/TA with KMP, (3) KHE/TA without KMP (Table 2). 7,22,24,29,30 Fulminant kaposiform hemangioendothelioma with Kasabach-Merritt phenomenon in a neonate/young infant Patients in this archetype typically present in extremis and require intensive management for cardiovascular instability, respiratory compromise, or severe KMP potentially with bleeding. 22,31 In some cases, recognition of the KHE lesion may be delayed because it is limited to the retroperitoneal region and there are no supportive physical exam cues for providers. ...

On Response of Tufted Angiomas to Low-Dose Aspirin
  • Citing Article
  • January 2014

Pediatric Dermatology

... The formulations of colloidal oatmeal are offered in various forms such as bath treatments, cleansing bars, body washes, shampoos, lotions, creams, and shaving gels [59]. It is also a common ingredient in many commercial moisturizers that are designed to combat dry skin and associated itching, and it is especially beneficial for conditions such as AD [60]. ...

Natural Ingredients in Atopic Dermatitis and Other Inflammatory Skin Disease
  • Citing Article
  • September 2013

Journal of Drugs in Dermatology

... The HOME initiative has agreed upon clinician-reported signs, patient-reported symptoms, quality of life, and long-term control as the core domains to measure for AE trials [1][2][3]. Guided by the assessments of the measurement properties of instruments available to measure these domains, consensus processes identified instruments for each domain [1,[3][4][5][6]. COSs are needed for optimal comparison and combination of trial data in order to make informed decisions that drive improved patient care. ...

Towards global consensus on outcome measures for atopic eczema research: Results of the HOME II meeting
  • Citing Article
  • July 2012

... Similarly to yellow light at 595 nm, this wavelength is well absorbed by oxyhemoglobin but, unfortunately, even more strongly by melanin. This affects the penetration depth [21] and increases the probability of scarring. Due to the smaller penetration depth, these lasers are most efficient for treating superficial vascular lesions, including capillary malformations. ...

Facial Port-Wine Stain: When to Worry?
  • Citing Article
  • January 2012

Pediatric Dermatology

... Isotretinoin is absolutely contraindicated in pregnancy and lactation, requiring strict contraception during treatment and for one month afterward [68]. Common side effects like skin dryness (72.13%), cheilitis (94.25%), dry eyes (29.49%), and muscle aches (23.05%) are reversible and dose-dependent [228]. Muscle aches can sometimes be associated with elevated creatine phosphokinase (CPK) levels, indicating potential muscle damage [229][230][231][232]. ...

Effective monitoring of isotretinoin safety in a pediatric dermatology population: A novel "patient symptom survey" approach
  • Citing Article
  • May 2011

Journal of the American Academy of Dermatology