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Aug 2018




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Thanking you
With sincere regards
Dr. Rajendra Kumar Ghritlaharey, M.S., M. Ch., FAIS
Associate Professor,
Department of Paediatric Surgery, Gandhi Medical College & Associated
Kamla Nehru & Hamidia Hospitals Bhopal, Madhya Pradesh 462 001 (India)
E-mail: drrajendrak1@rediffmail.com
On May 11,2011




Dr. Shankar P.R.

"On looking back through my Gmail archives after being requested by the journal to write a short editorial about my experiences of publishing with the Journal of Clinical and Diagnostic Research (JCDR), I came across an e-mail from Dr. Hemant Jain, Editor, in March 2007, which introduced the new electronic journal. The main features of the journal which were outlined in the e-mail were extensive author support, cash rewards, the peer review process, and other salient features of the journal.
Over a span of over four years, we (I and my colleagues) have published around 25 articles in the journal. In this editorial, I plan to briefly discuss my experiences of publishing with JCDR and the strengths of the journal and to finally address the areas for improvement.
My experiences of publishing with JCDR: Overall, my experiences of publishing withJCDR have been positive. The best point about the journal is that it responds to queries from the author. This may seem to be simple and not too much to ask for, but unfortunately, many journals in the subcontinent and from many developing countries do not respond or they respond with a long delay to the queries from the authors 1. The reasons could be many, including lack of optimal secretarial and other support. Another problem with many journals is the slowness of the review process. Editorial processing and peer review can take anywhere between a year to two years with some journals. Also, some journals do not keep the contributors informed about the progress of the review process. Due to the long review process, the articles can lose their relevance and topicality. A major benefit with JCDR is the timeliness and promptness of its response. In Dr Jain's e-mail which was sent to me in 2007, before the introduction of the Pre-publishing system, he had stated that he had received my submission and that he would get back to me within seven days and he did!
Most of the manuscripts are published within 3 to 4 months of their submission if they are found to be suitable after the review process. JCDR is published bimonthly and the accepted articles were usually published in the next issue. Recently, due to the increased volume of the submissions, the review process has become slower and it ?? Section can take from 4 to 6 months for the articles to be reviewed. The journal has an extensive author support system and it has recently introduced a paid expedited review process. The journal also mentions the average time for processing the manuscript under different submission systems - regular submission and expedited review.
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Dr. P. Ravi Shankar
KIST Medical College, P.O. Box 14142, Kathmandu, Nepal.
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On April 2011
Anuradha

Dear team JCDR, I would like to thank you for the very professional and polite service provided by everyone at JCDR. While i have been in the field of writing and editing for sometime, this has been my first attempt in publishing a scientific paper.Thank you for hand-holding me through the process.


Dr. Anuradha
E-mail: anuradha2nittur@gmail.com
On Jan 2020

Important Notice

Original article / research
Year : 2023 | Month : January | Volume : 17 | Issue : 1 | Page : WC01 - WC05 Full Version

Clinical Characteristics of Photodermatoses in Indian Patients and their Phototesting Findings: A Cross-sectional Study


Published: January 1, 2023 | DOI: https://doi.org/10.7860/JCDR/2023/59819.17295
Aishwaria Suresh, TP Thankappan

1. Assistant Professor, Department of Dermatology, KMCT Medical College, Calicut, Kerala, India. 2. Professor, Department of Dermatology, Pushpagiri Medical College, Thiruvalla, Kerala, India.

Correspondence Address :
Dr. Aishwaria Suresh,
Assistant Professor, Department of Dermatology, KMCT Medical College, Calicut-673602, Kerala, India.
E-mail: aishwariasuresh@gmail.com

Abstract

Introduction: Phototesting helps to confirm photosensitivity, identify the action spectra, reproduce lesions by photo provocation for biopsy, calculate starting dose of desensitisation therapy, assess the severity of the photodermatoses, and monitor response to treatment. The effect of sunlight on darker skin has only been sparingly studied and hence, this study was undertaken in our population.

Aim: To identify the spectrum of photodermatoses, with their clinical characteristics and phototesting findings.

Materials and Methods: A cross-sectional study was conducted in Outpatient Department (OPD) of the Department of Dermatology, Pushpagiri Medical College, Tiruvalla, Kerala, India from January to December 2015. A total of 30 patients clinically diagnosed as photodermatoses were subjected to phototesting using the whole body phototherapy unit with Ultraviolet A (UVA) and UVB exposure. After 24 hours the UV-exposed areas were examined for the Minimal Erythema Dose (MED), and for the reoccurrence of skin lesions to determine the action spectra for the disorder, and the values were expressed in mean, frequency, and percentage.

Results: Polymorphic Light Eruption (PLE) remains the most common photodermatosis (n=25) with a definite female preponderance (n=19). The mean MED-UVB for type IV skin with photodermatoses was found to be 766 mj/cm2 and for type V skin was found to be 900 mj/cm2. MED-UVA was not observed in the majority of patients (n=24). Among the 25 patients with PLE, 16 patients had normal MED values to both UVA and UVB, four had reduced MED-UVB alone, one patient to UVA alone, and three patients had reduced MED to both. MED-UVB was not observed in one patient. MED-UVA was not observed in 21 patients (normal). Of the three patients with photoallergic dermatitis, one patient had reduced MED-UVB and MED-UVA. The other two patients had normal MEDs. The chronic actinic dermatitis patient had reduced MED to UVB and UVA and the actinic lichen planus patient had normal MEDs.

Conclusion: Phototesting remains a very useful tool in the evaluation and management of photodermatoses and PLE was the most common photodermatoses in studied population.

Keywords

Polymorphic light eruption, Photosensitivity, Phototherapy

Photodermatoses are disorders of the skin characterised by an abnormal cutaneous response to ordinary light exposure (1). Erythema is the most visually apparent indicator of UV-induced skin inflammation. Erythema has been used as the endpoint for measuring the relative effects of UVB and sometimes of UVA, usually expressed as the action spectrum (2). The effect of sunlight on darker skin has only been sparingly studied (3),(4). The effect of sunlight does depend on the skin colour, skin type, and type of melanin in the skin (4). Photodermatoses are common in the Indian population despite the better natural photoprotection offered by melanin (4). Phototesting helps to confirm photosensitivity (5), identify the action spectra, reproduce lesions by photoprovocation for biopsy (3), calculate starting dose of desensitisation therapy, assess the severity of the photodermatoses and monitor response to treatment (5).

In India, the incidence of photodermatoses is high in view of the tropical weather, lack of knowledge regarding sun protection, and inadvertent consumption of phototoxic drugs (6). Identification of the cause and avoidance of triggering factors will help in reducing the incidence of photodermatoses (6). This study intends to identify the spectrum of photodermatoses with their clinical characteristics and phototesting findings and to find out the minimal erythema dose in these patients by UVA and UVB irradiation.

Material and Methods

A cross-sectional study was conducted in the Department of Dermatology, Pushpagiri Medical College, Kerala, India from January to December 2015. A total of 30 patients attending OPD with photodermatoses during the stipulated period of study duration were included in the study, after obtaining ethical committee clearance (PIMSRC/E1/388A/12/2015) and patient consent.

Inclusion criteria: Patients clinically diagnosed to have photodermatoses based on distribution of skin lesions on or predominantly on sun exposed areas, and patients willing to undergo the phototesting procedure, which takes about an hour in the phototherapy unit were included in the study.

Exclusion criteria: Patients with severe photosensitivity with dissemination of lesions to large areas and pregnant women were excluded from the study.

Study Procedure

The patient’s clinical characteristics and Fitzpatrick’s skin types, (Table/Fig 1) (7) were recorded and they were then subjected to phototesting in the active stage before initiation of the treatment.

‘Daavlin 3 series SPTM and 3 series PCTM Full body phototherapy device with smart touch control system, model number 311/350-24/24’ was used for the purpose of phototesting. The device is equipped with 24 lamps that emit UVA (peak 350 nm) and 24 Narrow Band UVB/TL-01 lamps (peak 311 nm). A full length gown with full sleeves was worn by the patient (Table/Fig 2). 4 cm2 openings were put on the back of the gown, six on each side, for UVA and UVB exposure (Table/Fig 3). Eyes were protected with UV blocking goggles and the face was covered with a cloth. Areas to be exposed were marked with a marker pen (Table/Fig 4).

Patients were then subjected to sequentially higher doses of UV light exposure on 4 cm2 area of the upper back. UVA was exposed at doses of 2,4,8,12,16 and 20 j/cm2 (Table/Fig 5). UVA dose of 2 j/cm2 was initially applied on the back. The first opening on the back of the gown was then closed. 2 j/cm2 was applied again, so that, a total of 4 j/cm2 is received at the second opening, which was then closed, and the process was repeated till all the openings received the required doses. UVB was also similarly exposed at doses of 200, 400, 600, 800, 1000 and 1200 mj/cm2.

After 24 hours the UV exposed areas were examined for the minimal erythema dose, and for reoccurrence of skin lesions to determine the action spectra for the disorder.

Statistical Analysis

Statistical analysis was done using epi info 7 software. The continuous variables like age, duration of disease, time from sun exposure to development of lesions etc were summarised as mean and standard deviation. The type of photodermatoses and sensitivity to UVA or UVB was expressed in frequency and percentage.

Results

A total of 23 females and 7 males were included in the study. Majority of the participants were in 41-50 years of age (Table/Fig 6). The mean age was 43 years.

PLE remains the most common photodermatoses (n=25), with a definite female preponderance [Table/Fig-7,8]. None of the patients had a family history of PLE. About 14 patients with PLE had recurrent episodes of the disease. Most of the patients (n=26,86.6%) diagnosed to have photodermatoses were involved in indoor works. They were incidentally exposed to sunlight for different purposes like hanging clothes, travel to work place etc. Only four patients were involved in regular outdoor works. Sixteen patients developed lesions after exposure to afternoon sun, nine after exposure in the morning, four in the evening and one patient after exposure to a newly installed CFL in the office (Table/Fig 9). Most patients (n=18) developed the disease within 7-24 hours of exposure to light, six patients within six hours, five patients after 24 hours and time of onset was unnoticed by one patient. The patient with chronic actinic dermatitis had a history of parthenium dermatitis earlier while residing in North India. There was a definite seasonal exacerbation in summer for 66.7% patients (Table/Fig 10).

Majority of patients were of Fitzpatrick’s skin type IV (n=23), six patients were of skin type V and remaining one patient was of skin type III. The mean MED-UVB (minimal erythema dose to ultraviolet B) for type IV skin with photodermatoses was found to be 766 mj/cm2 and for type V skin was found to be 900 mj/cm2. MED-UVA was not observed in the majority of patients (n=24). Among the 25 patients with PLE, 16 patients had normal MED values to both UVA and UVB, four had reduced MED-UVB alone (Table/Fig 11), one patient to UVA alone, three patients had reduced MED to both. MED-UVB was not observed in one patient and MED-UVA was not observed in 21 patients (normal). In the three patients with photoallergic dermatitis, one patient had reduced MED-UVB and MED-UVA. Other two patients had normal MEDs.The chronic actinic dermatitis patient had reduced MED to UVB and UVA (Table/Fig 12) and the actinic lichen planus patient had normal MEDs.

Discussion

The PLE was the most common photodermatosis observed in present study population (83.3%), followed by photoallergic dermatitis. In a study from India it has been found to be 0.56% in the plains and as high as 3.81% in hilly areas (8). PLE was the most common photodermatoses reported in previous studies also (1),(9),(10),(11). The mean age of PLE patients was 43 years in present study which was higher than a previous study from India (32.7 years) (1). The female predominance in PLE is well documented (12),(13),(14) as in present study (n=19,76%). About 14 (56%) of the patients with PLE had recurrent episodes of the disease in present study. None of the patients had a family history of PLE even though it is reported in upto one sixth of patients in literature (15). Most patients with PLE developed the disease after 6-24 hours of exposure to light, five patients within six hours, four patients after 24 hours and time of onset was unnoticed by one patient. One patient who developed the lesions after 6-24 hours had no history of sun exposure but developed after installation of a new CFL in office. PLE is a delayed type of hypersensitivty response and is reported to occur between 30 minutes to three days after exposure to sunlight (15). Flourescent lighting has been shown to induce lupus erythematosus lesions and chronic actinic dermatitis and has the potential to induce other idiopathic photodermatoses like PLE but to what extent is not yet clear (16). Two-third of patients (n=16) had disease onset in summer, followed by disease occurrence in summer and spring. Onset or worsening of PLE in summer and spring is reported. Among the patients with PLE 32% had low MED responses. Four had reduced MED-UVB alone, one patient had reduced MED-UVA alone and three patients had reduced MED to both. Around 15-30% abnormal MED responses have been documented in literature (17),(18) and the incidence was slightly higher in this study. MED-UVB was not observed in one patient. This could probably be due to a MED above the test ladder that was employed, that is, above 1200 mj/cm2. Higher than normal MED values have also been reported for PLE patients (19). Rest of the 16 patients (64% of patients) had normal minimal erythemal responses, the incidence was slightly lower than that in previous studies. Que SKT et al., reported 68% (n=216) of their PLE patients to have normal MED responses to UVB, UVA and visible light (10). Magnus IA (20) in 1964 and Frain-Bell W et al., (21) also had reported normal MED in PLE patients earlier.

Of the three PAD patients, one patient had reduced MED-UVA and UVB, other two patients had normal MEDs. The patient with systemic PAD due to Non Steroidal Anti-Inflammatory Drugs (NSAIDs) intake had the reduced MED. In the CAD patient MED to UVB and UVA was reduced as in previous studies (1),(17). In the absence of abnormal phototests a diagnosis of CAD cannot be made (18). Actinic lichen planus patient had normal MEDs as in a previous case (22). All the patients with PAD, and six patients with PLE were using different topical applications on the involved sites. Of these, four patients with PLE were using sandalwood soaps which is a known photosensitiser that might have predisposed them to development of disease (23). One patient with PAD probably had systemic photoallergic dermatitis due to NSAID use (the patient was also using medicated oils) and the other two had photocontact allergic dermatitis from face pack and fairness creams. The sunscreen incorporated in the fairness cream or fragrance in face pack might have induced photosensitivity in the patients here, but the exact composition could not be assessed. The most common lesions in this study were irregular papules and plaques with scaling and erythema.

Only one patient had chronic actinic dermatitis and one had actinic lichen planus both of which are reported to be less common (12). The patient with chronic actinic dermatitis had a history of parthenium dermatitis earlier while residing in North India. There is a definite trend towards a change from an airborne pattern to a CAD pattern in the natural history of parthenium dermatitis (24). In actinic lichen planus, skin tests for ultraviolet sensitivity are reported to be negative in most cases. Therefore, the cause of the occurrence of eruptions exclusively on the light-exposed areas remains unclear (25).Verhagen AR and Koten JW hypothesised that light induces the Koebner phenomenon that progresses to actinic lichen planus in a certain population of patients who have a tendency to develop lichenoid eruptions (26).

There were no patients with idiopathic photodermatoses like actinic prurigo, hydroavacciniforme and solar urticaria as in other case series from India (1) as they are very rare in our country. There are no Indian studies on MED in patients with photodermatoses. Considering the two studies from India on normal skin by Pai GS et al., (27) and Tejasvi T et al., (28) an average value of 800 mj/cm2 for type IV skin and 925 mj/cm2 for type V skin was considered normal in present study. In present study, seven patients with type IV skin had a MED-UVB less than 800 mj/cm2 and two patients with type V skin had MED-UVB less than 925 mj/cm2 (600 mj/cm2 and 800 mj/cm2) which was low. Mehta RV et al., (3) from India could not demonstrate erythema to UVA in type IV and type V skin even after irradiation upto 700 j/cm2 with a solar simulator. Hence, it is proposed that the MED for UVA on Indian skin is probably greater than 700 j/cm2. In present study, six patients with photodermatoses had observable erythemal response to UVA at less than 20 j/cm2 which was abnormal.

Limitation(s)

Small sample size due to the prolonged time required for phototesting in the phototherapy unit.

Conclusion

Polymorphic Light Eruption (PLE) remains the most common photodermatoses and phototesting findings are normal in a majority of patients with PLE. This study emphasises the importance of using phototests in conjunction with a history and physical examination, in conforming the diagnosis, identify those wavelengths of light which are most detrimental to an individual patient, and hence to take adequate measures to prevent exposure to those wavelengths of light.

References

1.
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DOI and Others

DOI: 10.7860/JCDR/2023/59819.17295

Date of Submission: Aug 26, 2022
Date of Peer Review: Sep 23, 2022
Date of Acceptance: Nov 12, 2022
Date of Publishing: Jan 01, 2023

AUTHOR DECLARATION:
• Financial or Other Competing Interests: None
• Was Ethics Committee Approval obtained for this study? Yes
• Was informed consent obtained from the subjects involved in the study? Yes
• For any images presented appropriate consent has been obtained from the subjects. Yes

PLAGIARISM CHECKING METHODS:
• Plagiarism X-checker: Sep 05, 2022
• Manual Googling: Nov 05, 2022
• iThenticate Software: Nov 11, 2022 (8%)

ETYMOLOGY: Author Origin

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