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제목	A Clinical Study on Combined Therapy in Lepromatous Leprosy


저자	Hae Young Lee, Do Il Kim	소속	Institute for Leprosy Research, Korean Leprosy Association, Anyang, Korea

년도	1983	권	16

호	1	번호

시작페이지	21	끝페이지	47

첨부

요약	It is now widely recognised that the serious problems in leprosy control programmes have been encountered by the widespread emergence of DDS-resistant strains of Mycobacterium leprae among lepromatous patients who have been treated with DDS monotherapy, and among those infected from DDS-resistant cases and it is generally agreed that the only potentially successful method of preventing the present situation from becoming more serious is to initiate the treatment of all new and relapsed lepromatous patients with combination of at least two or more anti-leprosy drugs. The followings are the results of our clinical study on combined therapy in lepromatous leprosy. 1. Combined therapy with regimen I-A (DDS 100mg daily ×－＋ Rifampicin 1,200mg single dose) was given to 10 previously untreated DDS-sensitive new lepromatous patients and the following results were obtained with 48 months' observation. (1) Skill lesions were shown definite improvement in all cases. (2) Neurological findings and disability were shown slight improvement. (3) In skin smears, MI declining was rather slow than in I-D trial group and it took about 12 months to become MI 0%, and BI was decreased only 0.7＋ during 48 months' treatment. (4) 79% of trial cases had occurred ENL reaction at about six months after initiation of treatment. (5) There were no severe drug allergy and toxicity and well-tolerated in all cases. 2. Combined therapy with I-D (DDS 100mg daily ×－＋ Rifampicin 1,200mg single dose Prothionanlide 375 mg daily × 8 weeks) was given to 15 previously untreated DDS-sensitive new lepromatous patients and the following results were obtained with 36 months' observation. (1) Skin lesions were shown definite improvement in all like in I-A trial group. (2) Neurological findings and disability were shown moderate improvement which is better than in I-A trial group. (3) In skin smears, MI declining was quicker than in I-A trial group and it tools about 9 months to become MI 0%, tut BI Ivas not decreased during 20 months' treatment. (4) 60% of this trial group had occurred ENL reaction at about 12 months after initiation of treatment. (5) Many patients had high units of SGPT after taking prothionamide, but it became normal after stop prothionamide. 3. Combined therapy with Ⅱ-A (Clofafimine 50mg daily ×－＋ Rifampicin 600mg daily × 4 weeks) was given to 9 proven DDS-resistant relapsed lepromatous patients and the following results were obtained with 18 months' observation. (1) Skin lesions were shown definite improvement in all cases. (2) Neurological findings and disability were shown gradual deterioration in all. (3) In skin smears, MI declining was relatively rapid and it took about 9 months to become MI 0%, and BI was decreased 0.8＋after 18 months' treatment. (4) 44% of this trial cases had occurred ENL reaction at about 9 months after initiation of treatment. (5) As side-effects of regimen, skin pigmentation and xeroderma had appeared in all cases. This is mainly due to clofazimine intake. 4. Combined therapy with Ⅱ∼D (Rifampicin 600mg daily×8 weeks, afterwards 600mg daily × 2 consecutive days monthly ×－＋ prothionamide 375mg daily × 8 weeks and then Thiacetazone 150mg daily ×－) was given to 6 proven DDS-resistant relapsed lepromatous patients and the following results were obtained with 18 months' observation. (1) Skin lesions were shown definite improvement in all cases. (2) Neurological findings and disability were shown gradual deterioration like in Ⅱ-A group. (3) In skin smears, fill declining was rapid like Ⅱ-A group and it took average 9 months to become MI 0%, and BI was rather increased unlikely in Ⅱ-A trial group. (4) 50% of this trial group had occurred ENL reaction at six months after initiation of treatment. (5) Some cases had high unit of SGPT without clinical symptoms. This is probably due to either prothionamide or thiacetazone.

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