Efficacy Of Dapsone Research Articles

P10 Collapse, confusion and acute kidney injury presenting in the context of bullous skin disease in a young male patient

P10 Collapse, confusion and acute kidney injury presenting in the context of bullous skin disease in a young male patient

Dapsone in Hidradenitis Suppurativa: A Systematic Review.

IntroductionHidradenitis suppurativa (HS) is a chronic, inflammatory, recurrent disease, usually presenting after puberty with inflammatory lesions that mainly affect the apocrine gland-bearing areas of the body, most commonly the axillary, inguinal and anogenital regions. The treatment of HS is associated with certain challenges due to intrinsic resistance to various treatments and the presence of comorbidities and complications. The antibiotic dapsone is an established treatment for HS, but the current evidence base is limited. The aim of this review is to systematically review the literature on the efficacy of dapsone in the treatment of HS.MethodsThe Cochrane, PubMed and CINAHL databases were searched for relevant articles to be included in the systematic review.ResultsA total of seven studies, with a cumulative patient population of 135 patients, were included. Of these 135 patients, 62.2% demonstrated various degrees of improvement following treatment. However, as only three of the seven studies used dapsone monotherapy it is difficult to assess the effectiveness of dapsone because the benefits observed may be due to concurrently administered treatment.ConclusionOverall, the quality of evidence supporting the use of dapsone is weak. However, it is a well established treatment recommended in current, various national guidelines. There is a crucial need for well-designed randomized controlled trials to support its usage.

Efficacy of dapsone in a pediatric IgA vasculitis patient with steroid and therapy-resistant abdominal pain: A case report with literature

Efficacy of dapsone in a pediatric IgA vasculitis patient with steroid and therapy-resistant abdominal pain: A case report with literature

WITHDRAWN: Biodegradable Self-assembled polymeric Micelles based on Poly (ethylene oxide)-block-Polylactide block copolymer for sustained delivery of dapsone

Dapsone is the simplest antibiotic of sulphones that demonstrates its viability against various species of bacteria and protozoa. By restricting dihydrofolic acid synthesis through competition with para-amino benzoate, dapsone inhibits the growth of these microorganisms. Owing to its low aqueous solubility and non-specific distribution in the body, the applicability of dapsone is impeded. A control on pharmacokinetics and targeted delivery of drugs is deeply needed in order to reduce the side effects of the drug and make treatment more progressive. The aim of this study is to increase the bioavailability and efficacy of dapsone through the delivery of MeO-PEO 5K -b-PLA micelles. The effect of the length of the hydrophobic block (PLA) on micelles size, critical micelle concentration, entrapment efficiency, and release study is assessed. The PMs were prepared using the solvent evaporation process. The CMC of synthesized block copolymer was measured using a fluorescence-based method. The size and morphology of PMs was determined by dynamic light scattering (DLS) and atomic force microscopy (AFM). The entrapment efficiency and release kinetic behavior of MeO-PEO 5K -b-PLA based PMs were determined by UV-visible spectroscopy and dispersion method, respectively. The size of micelles increased and the rate of drug release decreased as the length of the PLA block increased. With copolymers having greater PLA block length, the maximum encapsulation efficiency of 89.58 percent for dapsone is attained. A comparison of dapsone's antibacterial activity against S. Aureus is performed and delivered by PMs. In comparison to pure drugs, the MIC for PMs loaded with dapsone has decreased. Morphological analysis based on AFM also verified the decrease in MIC.

Oral dapsone for the treatment of generalized granuloma annulare: A retrospective case series

Oral dapsone for the treatment of generalized granuloma annulare: A retrospective case series

Efficacy of Dapsone 5% gel in treatment of Acne vulgaris

<p class="abstract"><strong>Background:</strong> Acne vulgaris is chronic inflammatory disorder of pilosebaceous unit mainly characterized by comedones, papules and nodulocystic lesions affecting face and upper trunk. Topical dapsone 5% gel is approved to treat acne vulgaris because of its anti-inflammatory and anti-bacterial activities.</p><p class="abstract"><strong>Methods:</strong> A single center, open label interventional study was conducted during 1 year period in dermatology OPD of Jawaharlal Nehru Medical College, Sawangi (Meghe), Wardha, Maharashtra. Patients were enrolled in the study considering inclusion criteria. Patients were asked to apply dapsone 5% gel twice daily on face for 12 week. Efficacy was evaluated by mean percent reduction in total, inflammatory and non-inflammatory lesions and success rate on change in investigator global acne severity assessment scale while tolerability was assessed by evaluating skin dryness, erythema, stinging or burning sensation and scaling at baseline, 1, 2, 4, 8 and 12 week.<strong></strong></p><p class="abstract"><strong>Results:</strong> At end of 12 week, success rate reached to 31.54%. Dapsone 5% gel was effective in reduction of total, non-inflammatory and inflammatory lesions by 57.75%, 52% and 63.1% respectively. Side effects with dapsone gel were tolerable, mild and transient.</p><p><strong>Conclusions:</strong> Dapsone 5% gel was efficacious and well tolerated in non-inflammatory as well as inflammatory acne lesions. </p>

OI0441 Efficacy of dapsone and sulfamethoxypyridazine in the treatment of MMP

OI0441 Efficacy of dapsone and sulfamethoxypyridazine in the treatment of MMP

Wells syndrome: response to dapsone therapy.

Dear Editor: Eosinophilic cellulitis, known as Wells syndrome (WS), is a rare recurrent inflammatory skin condition that was first described by Wells in 19711. A number of therapies have been reported since then, including systemic and topical corticosteroids, cetirizine, interferon-α, griseofulvine, cyclosporine, and antimicrobial agents, with variable results. We report a case of WS that responded to treatment with dapsone. A 67-year-old woman presented with a severely itching rash, consisting of urticaria-like, infiltrating, red-violet plaques on the upper and middle back, abdomen, thighs, and submammary region (Fig. 1A). She reported having recurrent lesions during winter for the last 3 years. She denied any associated symptoms, drug intake, or insect bites. Her medical history included chronic obstructive pulmonary disease. In the past, she had been investigated for urticaria, with negative skin prick tests and radioallergosorbent test. Fig. 1 (A) An indurated red-violet plaque on the upper back upon admission. (B) Clearance of eruption two weeks after the administration of dapsone 100 mg/day. Complete blood count analysis revealed 19.8% eosinophils (reference range, 0%~2%). Level of eosinophil cationic protein was elevated in peripheral blood (192 µg/L; reference, <4.4 µg/L). Levels of urea and electrolytes, antinuclear antibodies, anti-DNA, and C3 and C4 complement, as well as the results of liver function tests and chest radiography were normal. A skin biopsy (Fig. 2) revealed a deep perivascular infiltration of lymphocytes and innumerable eosinophils. Collections of eosinophils with eosinophilic granules (flame figures) among collagen bundles were noted. On the basis of the clinical and histological findings, a diagnosis of WS was established. As the patient had received several courses of prednisolone in the past without any improvement, dapsone was initiated at a dose of 100 mg daily. She responded to this treatment within 2 weeks (Fig. 1B). Subsequently, the dose of dapsone was tapered to 50 mg daily for the next 6 months, with further clinical improvement and reduction of eosinophils (9%). The therapeutic regimen of dapsone was then modified to a dose of 50 mg administered thrice every week. At the last follow-up, 2 years after the initiation of treatment, she did not show the presence of lesions, eosinophils were within normal limits (2%), and the treatment was ceased. No adverse reactions were noted during this period. WS is primarily a disease in adults of any race and sex2. The etiology is unknown. However, there are several precipitating factors including insect bites; bacterial, viral, and parasitic infestations; and any type of drug. The disease usually presents with a mildly pruritic or tender cellulite-like eruption, with typical histological features characterized by edema, figures, and marked infiltration of eosinophils in the dermis. The management of WS is difficult and poses a therapeutic challenge. Fig. 2 (A) The presence of a flame figure is demonstrated in a diffuse infiltrate of eosinophils at the lower dermis (H&E, ×200). (B) Severe and diffuse dermal infiltrate of eosinophils and less in number lymphocytes and histiocytes (H&E, ... The efficacy of dapsone in WS has been poorly reported in the literature3,4. The exact mode of action of dapsone in WS is still unclear. It has antimicrobial, anti-inflammatory, and immunomodulating properties. It is known for its anti neutrophilic action through an inhibitory effect on myeloperoxidase. Additionally, it has been shown to inhibit of eosinophil peroxidase, which is a cytotoxic granule protein of eosinophils that induces mast cell degranulation5. Mast cells produce interleukin (IL)-5, a key mediator in eosinophil activation. IL-5, originally discovered as an eosinophilic colony-stimulating factor, is a major regulator of eosinophil accumulation in tissues that can modulate eosinophil behavior at every stage, from maturation to survival. Considering that eosinophils are the primary IL-5RA-expressing cells, the above mentioned properties of dapsone might account for its beneficial effects in the therapy of WS. Dapsone is effective and well tolerated in low doses by most patients. In addition, it is inexpensive and safer for long-term treatment compared with corticosteroids and other immunosuppressive agents. Our data suggest that dapsone at low doses can be used for long periods to control long-term WS.

Outcome of Dapsone in the Treatment of Ashy Dermatosis

Background: Ashy dermatosis or Erythema Dyschromicum Perstans is a rare disorder of unknown etiology characterized by asymptomatic,slowly progressive, ashen-gray macular pigmentation of the skin. Various therapies have been tried without any benefit. The anti-inflammatory activity of dapsone on Erythema Dyschromicum Perstans may be the first oral treatment option. Objective: The aim of the present study was to evaluate the efficacy of dapsone in the treatment of ashy dermatosis. Methodology: This study was carried out on total thirty (30) cases having ashy dermatosis &amp; age group 20-60 years were selected for the study of which 16 females &amp; 14 males during the period of January 2010 to December 2011 in the Department of Dermatology &amp; Venereology of Shaheed Suhrawardy Medical College Hospital and Bangabandhu Sheikh Mujib Medical University at Dhaka city of Bangladesh. All the cases were diagnosed clinically &amp; confirmed by histopathological examination. The patients were given Dapsone 100 mg daily for three months &amp; follow up was done for the next 3 months. Results: 16(53.33%) females &amp; 14(46.66%) males were included in the study. Out of thirty patients, two patients (6.66%) shown excellent response, seven patients (23.33%) shown good response, eight (26.66%) patients shown fair response, 8 patients (26.66%) shown poor response &amp; remaining five patients (16.66%) did not show any response clinically. So improvement was shown in 25(83.33%) cases and 5(16.66%) cases show no improvement at all. Conclusion: This study suggests that dapsone has significant efficacy profile for treatment option of ashy dermatosis. DOI: http://dx.doi.org/10.3329/jssmc.v4i1.11998 J Shaheed Suhrawardy Med Coll, 2012;4(1):18-21

Simple HPLC determination of the concentrations of epiroprim in the serum and brains of mice.

Epiroprim, an analogue of trimethoprim, has been shown to potentiate the efficacy of dapsone in experimental parasitic infections. A simple and accurate HPLC method has been developed to estimate epiroprim in serum and brain. Blood and brains from mice were sampled 0, 30, 75, 120 and 240 min after 50 or 100 mg kg-1 oral gavage. The drug and added internal standard metoprine in serum and brain supernatant were isolated by solid-phase extraction (Superclean LC-SCX). The HPLC system consisted of a 150 x 4.6 mm Hypersil 5 microns ODS column. The mobile phases contained various proportions of acetonitrile, methanol and phosphate buffer (0.1 M). Peaks were detected by UV absorbance at 210 nm. Serum concentrations (mean +/- s.e.m.) of epiroprim were highest at 30 min for both 50 and 100 mg kg-1 doses, 173 +/- 20 and 207 +/- 25 ng mL-1, respectively, falling to 8 +/- 5 and 18 +/- 6 ng mL-1, respectively, at 240 min. Epiroprim concentrations in the brain correlated well with those in the serum, with levels of 223 +/- 69 and 265 +/- 21 ng g-1 falling to 10 +/- 10 and 31 +/- 11 ng g-1, respectively. Epiroprim is rapidly absorbed and distributed to the brain.

Efficacy of Dapsone in the Treatment of Pemphigus and Pemphigoid

Dapsone is a chemotherapeutic agent primarily used in treating leprosy, Pneumocystis jiroveci (previously carinii) pneumonia, and malaria. It is also used as an adjuvant in the treatment of pemphigus and pemphigoid. To assess the role of dapsone in the treatment of pemphigus and pemphigoid, a retrospective review of reports in the English-language literature was conducted. Information on the number of patients treated, their average age, prior therapies, indications for use, protocol (dose and interval) used, concomitant therapies, reported adverse effects, and clinical outcomes were analyzed. There were 35 case reports/series published describing the use of dapsone in a total of 427 patients. Data on 55 pemphigus patients were obtained from several case reports and some case series and one randomized controlled trial. Of these, 32 patients with pemphigus vulgaris and 14 patients with pemphigus foliaceus responded to dapsone. Data from 13 case series, each including at least five patients, accounted for 372 patients with pemphigoid. The overall response rates to dapsone, when given either alone or in combination with corticosteroids or immunosuppressive agents, were 84% in mucous membrane pemphigoid, and 81% in bullous pemphigoid. Hemolysis was the most common adverse effect observed. Dapsone is a promising and useful agent in patients with autoimmune mucocutaneous blistering diseases, especially in mucous membrane pemphigoid. It can be used as a corticosteroid-sparing agent. Therefore, its combined use with oral corticosteroids may be useful in pemphigus vulgaris and bullous pemphigoid. Adverse effects of dapsone are dose dependent and usually reversible. Hemolysis and concomitant anemia secondary to hemolysis are expected in most patients. In the opinion of the authors, dapsone is underutilized in the treatment of autoimmune mucocutaneous blistering diseases.

Efficacy and safety of dapsone as a second-line treatment in non-splenectomized adults with immune thrombocytopenic purpura

In adults with immune thrombocytopenic purpura (ITP), steroids are usually proposed as first-line therapy, but long-term complete responses are obtained in no more than 20% of patients. For the remaining patients, splenectomy is considered the treatment of choice, with reported “cure” rates from 60–70%. However, the inherent risks of surgery and sepsis after splenectomy without a guarantee of success justify the search for strategies aimed to avoid splenectomy. Here we retrospectively evaluated the results of dapsone treatment in ITP patients that failed first-line therapy with steroids. These patients received dapsone 100 mg/day for a minimum of 30 days before splenectomy was considered. Efficacy was defined as a sustained rise in platelet counts (>50 × 109/l) clearly attributed to dapsone treatment. Among 52 steroid-dependent or refractory patients, dapsone resulted in sustained increases in platelet counts in 44.2% of patients, after a median follow-up of 21.10 months after treatment initiation. The long-term efficacy of dapsone in this setting is further corroborated by the observation that none of the “responding” patients required splenectomy in the follow-up, compared to 69.0% of the “non-responding” patients. Dapsone-related adverse events were mild and promptly reversed by treatment withdrawal. The results of our retrospective analysis suggest that dapsone is a safe and effective second-line agent for steroid-dependent or refractory ITP patients. Because of its well-known safety profile and low cost compared to other potential second-line treatments for ITP, a trial course of dapsone should be viewed as an attractive option before splenectomy in steroid-dependent of refractory adult ITP patients.

Efficacy of Dapsone in Disseminated Granuloma Annulare: A Case Report and Review of the Literature

Granuloma annulare is a dermatosis of unknown cause that is generally self-limiting and has several clinical forms of presentation. It may be associated with pruritus or present asymptomatically. The disseminated variant of the disease accounts for 15% of all cases. Most authors consider that the duration of this form is longer and that treatment response is worse than for localized forms. A range of therapeutic options have been tried for this disease with a wide range of outcomes. We present a patient with disseminated granuloma annulare who started treatment with dapsone after several therapeutic failures. With dapsone therapy, her cutaneous symptoms showed a clear improvement without any relevant side effects. We then review reports in the literature of cases of disseminated granuloma annulare treated with dapsone.

Toxicity and Efficacy of Daily Dapsone as Pneumocystis jiroveci Prophylaxis after Hematopoietic Stem Cell Transplantation: A Case-Control Study

The toxicity and efficacy of dapsone given daily as Pneumocystis jiroveci (PCP) prophylaxis in hematopoietic stem cell transplant (HSCT) recipients who cannot take trimethoprim-sulfamethoxazole (TMP-SMX) have not been fully evaluated. We compared 155 HSCT recipients who received daily dapsone as second-line PCP prophylaxis with 310 matched control patients who received TMP-SMX throughout the posttransplantation course. Among patients who started dapsone before transplantation because of TMP-SMX allergy, there was no difference in the transfusion requirement after HSCT when compared with controls. Among patients who started dapsone after transplantation, increased red blood cell ( P < .0001) and platelet transfusion ( P = .003) requirements were noted compared with controls. This effect was, however, limited to patients who were receiving dapsone for reasons (mostly neutropenia) other than TMP-SMX allergy. Two of 155 patients developed PCP, compared with 0 of 310 controls ( P = .11); both patients survived. In conclusion, the efficacy of daily dapsone in preventing PCP was similar to that observed in patients able to remain on TMP-SMX prophylaxis. Dapsone did not seem to cause hematologic toxicity among TMP-SMX-allergic patients. The observed higher transfusion need in patients who received dapsone for reasons other than TMP-SMX allergy seems mostly due to an underlying condition of poor marrow reserve. Further studies are required to establish whether the drug has an etiologic role in these situations.

Maladie de Sneddon-Wilkinson. À propos de quatre cas

Introduction. – We report four cases of subcorneal pustular dermatosis or Sneddon-Wilkinson disease. Clinical and histological lesions and immunofluorescence data were presented. This disease is classified among neutrophilic dermatitis. Patients and methods. – All of four patients presented with clinical and histological lesions compatible with the diagnosis of Sneddon-Wilkinson disease. Indeed, direct and indirect immuno-testing were negative. We noted an association with a benign IgA monoclonal gammapathy in one case and with a seronegative polyarthritis in one other case. Three patients correctly responded to dapsone. One of them after transient improvement was resistant to dapsone and then dramatically responded to etretinate. Conclusion. – Subcorneal pustular dermatosis is a chronic disease, rarely described in literature. It’s a pustular eruption, involving the trunck, axillae and inguinal holds. It’s often associated with monoclonal gammapathy, particulary IgA. Its nosological situation is still contested, especially with IgA pemphigus sharing with it the association with IgA monoclonal gammapathy and the same efficacy of dapsone. We discuss relationships between both diseases.

PCP Prophylaxis in Patients Who Cannot Tolerate Bactrim

For patients who cannot tolerate trimethoprim or sulfonamides, dapsone and atovaquone offer equivalent protection against PCP. Trimethroprim-sulfamethoxazole (TMP/SMX) is the treatment of choice for prophylaxis against P. carinii pneumonia (PCP). However, intolerance to TMP/SMX is common, typically because of allergy. Although the efficacy of dapsone against PCP has been established, it is less effective than TMP/SMX when used prophylactically and is associated with a high rate of intolerance. Atovaquone is an agent that has proved effective …

Prevention and Early Detection of Leprosy in Children

India with its 4 million cases of leprosy, accounts for one-third of the world's population of leprosy patients. One-fourth of them are below 15 years of age. We report a 5-year follow-up study of healthy children who were close contacts of leprosy patients, in order to: 1. detect subclinical infection and observe the development of overt disease by using the Fluorescent Leprosy Antibody Absorption Technique (FLA-ABS) and the lepromin test which assess the humoral and cell-mediated immunity (CMI), respectively; 2. evaluate the efficacy of dapsone as a chemoprophylactic agent in the 'at risk' contacts. Four-hundred-and-fifty-five healthy contacts were studied. Majority of the contacts of multibacillary patients (303) were FLA-ABS positive (75 percent) and lepromin negative (55 percent) showing that although most of them had been infected, the lepromin status was negative (P < 0.01). On the other hand, the majority of the contacts of paucibacillary patients (152) were lepromin positive (57 percent) (P < 0.05). Furthermore, only 61 percent of contacts of paucibacillary patients were FLA-ABS positive as compared to 75 percent of contacts of multibacillary patients demonstrating that the former had been exposed to a lesser quantum of infection (P < 0.05). On the basis of results of FLA-ABS and lepromin tests, these 455 contacts were classified into four groups, viz. Group I comprising children who were FLA-ABS positive and lepromin positive; Group II, who were FLA-ABS positive and lepromin negative; Group III, who were FLA-ABS negative and lepromin positive; and Group IV who were FLA-ABS negative and lepromin negative.(ABSTRACT TRUNCATED AT 250 WORDS)

On the efficacy of dapsone in granuloma faciale.

The authors present a rare case of mycosis fungoides with early central nervous system involvement mimicking an intramedullary tumour in a 38- year-old white male.

Efficacy and safety of dapsone prophylaxis against Pneumocystis carinii pneumonia in human immunodeficiency virus-infected children.

Dapsone (4,4'-diaminodiphenylsulfone) is recommended as an alternative agent for prophylaxis against Pneumocystis carinii in children with human immunodeficiency virus infection. We reviewed our experience over the past 100 months with 20 children (age range, 2 months to 13 years) who received dapsone and examined the safety and efficacy of this regimen. Dapsone was taken for an average of 7.33 months/patient or a total of 4410 days by those children in whom safety could be assessed. Three of the 20 patients had an adverse reaction to dapsone. One had mild elevation of blood methemoglobin values (5.6%) and transient elevation of serum transaminases that resolved without discontinuing drug. The other two developed allergic skin rashes which necessitated discontinuation. Efficacy of dapsone in preventing P. carinii pneumonia (PCP) was assessed in 16 children at high risk for developing PCP (defined by CD4 counts or prior PCP infection). These 16 children took dapsone for an average of 6.88 months and a total of 3300 days. Two of the 16 high risk children, one who had had a previous P. carinii pneumonia, developed PCP while taking dapsone. Both had CD4 counts < or = 200 cells/mm3 and were taking dapsone for > or = 12 months before developing PCP. Dapsone is well-tolerated in children and appears to be as effective in preventing PCP in children with human immunodeficiency virus infection as it is in adults.

Anti-Toxoplasma effects of dapsone alone and combined with pyrimethamine

The efficacy of dapsone alone or combined with pyrimethamine against Toxoplasma gondii was investigated experimentally. For in vitro studies, a sensitive immunoassay was used for assessment of Toxoplasma growth in tissue cultures; dapsone was found to have a significant inhibitory effect at a concentration of 0.5 micrograms/ml in the cultures, and the 50% inhibitory concentration was estimated to be 0.55 micrograms/ml. When pyrimethamine and dapsone were combined, an important synergistic effect which was associated with morphological alterations of the parasites was observed. In vivo studies were performed in a murine model of acute toxoplasmosis in which a tissue culture method was used to estimate the parasite burden in the blood, lungs, and brains of infected mice. Dapsone alone, which was administered at 100 mg/kg/day for 10 days from day 1 after infection, was unable to prevent parasite dissemination and only delayed the time to death of treated mice compared with the time of death of untreated controls. When dapsone and pyrimethamine (18.5 mg/kg/day) were administered in combination from day 4 after infection, parasites were cleared from blood and organs within 6 days, but relapses were observed 15 days after the cessation of therapy. When treatment was started at day 1 after infection, 100% of mice survived and relapses were not observed, suggesting a good efficacy of this combination for preventive therapy.