PMID- 11854810
OWN - NLM
STAT- PubMed-not-MEDLINE
LR  - 20191120
IS  - 1536-3686 (Electronic)
IS  - 1075-2765 (Linking)
VI  - 2
IP  - 12
DP  - 1995 Dec
TI  - Misoprostol and Prednisone Treatment of Lupus Nephritis.
PG  - 928-932
AB  - Fourteen patients were enrolled in a placebo-controlled double-blind randomized 
      trial of 8 weeks of treatment for active lupus nephritis. Seven patients received 
      prednisone at a dose of 1 mg kg(minus sign1) day(minus sign1) plus misoprostol at 
      a dose of 200 &mgr;g P.O. Q.I.D.; 7 patients received prednisone plus placebo. 
      The patients included 12 females, 2 males; 3 African-Americans, 3 Asians, 5 
      Hispanics, and 3 Caucasians. There were no serious side effects associated with 
      prednisone or misoprostol treatment during the 8-week study period. Laboratory 
      measures obtained at baseline, 4, 8, and 12 weeks included complete blood count 
      (CBC), ESR, C reactive protein (CRP), serum creatinine, creatinine clearance, 
      24-h urine protein excretion, C3, C4, and anti-double stranded DNA (anti-dsDNA). 
      Statistical analysis was conducted assessing change in measures over time in the 
      entire study group by paired t-tests. The effect of treatment on change over time 
      was examined by analysis of covariance. Log transformation of the variables was 
      performed prior to statistical analysis. For the entire study group, the mean 
      levels of ESR, CRP, 24-h protein excretion, C3, C4, and anti-dsDNA were improved 
      at 4, 8, and 12 weeks. The mean ESR at baseline was 70 plus minus 8 compared to 
      42 plus minus 8 at 12 weeks (p < 0.01). The mean CRP at baseline was 0.6 plus 
      minus 0.2 compared to 0.2 plus minus 0.1 at 12 weeks (p < 0.01). The 24-h protein 
      excretion was 4367 plus minus 769 mg at baseline compared to 2512 plus minus 709 
      mg at 12 weeks (p = 0.02). The mean C3 at baseline was 40 plus minus 4 mg 
      dl(minus sign1) compared to 60 plus minus 4 mg dl(minus sign1) at 12 weeks (p < 
      0.01). The mean C4 at baseline was 14 plus minus 1 mg dl(minus sign1) compared to 
      23 plus minus 2 mg dl(minus sign1) at 12 weeks (p < 0.01). The mean anti-dsDNA at 
      baseline was 4268 plus minus 1780 compared to 316 plus minus 111 at 12 weeks (p < 
      0.001). The baseline serum creatinine (1.12 plus minus.15 mg dl(minus sign1)) and 
      creatinine clearance (82 plus minus 15 ml min(minus sign1)) were not 
      significantly changed at 12 weeks (1.10 plus minus 0.2 mg dl(minus sign1) and 80 
      plus minus 17 ml min(minus sign1), respectively). Comparing the misoprostol 
      treatment group to the placebo group, there were no statistically significant 
      differences for ESR, CRP, creatinine, creatinine clearance, 24-h protein 
      excretion, C3, C4, or anti-dsDNA at any time points. However, comparing the 
      misoprostol treatment group at 4 weeks to the placebo group, a more rapid 
      decrease in anti-dsDNA (reduction of 3297 plus minus 2374) was observed in the 
      misoprostol treatment group versus 304 plus minus 409 in the placebo group), as 
      well as lower mean anti-dsDNA levels (464 plus minus 140) in the misoprostol 
      treatment group versus 4118 plus minus 3834 in the placebo group). Also, the C3 
      and C4 levels at 12 weeks in the misoprostol treatment group (67 plus minus 5 and 
      27 plus minus 3 mg dl(minus sign1), respectively) were greater than levels in the 
      placebo group (52 plus minus 4 and 19 plus minus 3 mg dl(minus sign1), 
      respectively). The data demonstrate that oral prednisone is effective in reducing 
      proteinuria and improving the biological markers of disease activity (i.e., ESR, 
      CRP, C3, C4, and anti-dsDNA) following short-term treatment of active lupus 
      nephritis. Additionally, the more rapid change in anti-dsDNA levels and superior 
      normalization of complement levels in the treatment group, although not 
      statistically significant, are consistent with a biologic effect of misoprostol 
      on lymphocyte function and the production of a pathogenic autoantibodies.
FAU - Belmont, H Michael
AU  - Belmont HM
AD  - Department of Rheumatology, Hospital for Joint Diseases Department of Medicine, 
      New York University School of Medicine, New York, USA.
FAU - Kitsis, Elizabeth
AU  - Kitsis E
FAU - Skovron, Mary Louise
AU  - Skovron ML
FAU - Buyon, Jill
AU  - Buyon J
FAU - McCullagh, Eileen
AU  - McCullagh E
FAU - Abramson, Steven
AU  - Abramson S
LA  - eng
PT  - Journal Article
PL  - United States
TA  - Am J Ther
JT  - American journal of therapeutics
JID - 9441347
EDAT- 1995/12/01 00:00
MHDA- 2002/02/21 10:00
CRDT- 1995/12/01 00:00
PHST- 1995/12/01 00:00 [pubmed]
PHST- 2002/02/21 10:00 [medline]
PHST- 1995/12/01 00:00 [entrez]
AID - 10.1097/00045391-199512000-00005 [doi]
PST - ppublish
SO  - Am J Ther. 1995 Dec;2(12):928-932. doi: 10.1097/00045391-199512000-00005.