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Notes: Summary Previous studies have suggested an association between polymorphisms in the insulin gene region and insulin-dependent diabetes mellitus (IDDM). Most of the studies so far have been performed in Caucasoid populations. We have investigated 418 random IDDM patients and 422 healthy control subjects from three different ethnic groups; Tanzanian blacks, Norwegian Caucasians and Japanese orientals. Our data suggest that polymorphisms in the insulin gene region confer susceptibility to IDDM in Caucasians, and that a similar tendency though not statistically significant is observed among Tanzanian blacks, while no significant contribution is seen among Japanese orientals. We further demonstrate that the disease-associated genotype INS +/+ confers susceptibility independently of HLA class II alleles associated with IDDM. Compared to the contribution of particular HLA-DQ alleles in IDDM susceptibility, the additional risk conferred by the insulin gene region polymorphism is, however, small. Genotyping of the insulin gene region will therefore most probably not be a useful tool in the prediction of IDDM.

Notes: Summary Previous studies have suggested an association between polymorphisms in the insulin gene region and insulin-dependent diabetes mellitus (IDDM). Most of the studies so far have been performed in Caucasoid populations. We have investigated 418 random IDDM patients and 422 healthy control subjects from three different ethnic groups; Tanzanian blacks, Norwegian Caucasians and Japanese orientals. Our data suggest that polymorphisms in the insulin gene region confer susceptibility to IDDM in Caucasians, and that a similar tendency though not statistically significant is observed among Tanzanian blacks, while no significant contribution is seen among Japanese orientals. We further demonstrate that the disease-associated genotype INS+/+ confers susceptibility independently of HLA class II alleles associated with IDDM. Compared to the contribution of particular HLA-DQ alleles in IDDM susceptibility, the additional risk conferred by the insulin gene region polymorphism is, however, small. Genotyping of the insulin gene region will therefore most probably not be a useful tool in the prediction of IDDM. [Diabetologia (1994) 37: Wingdingsx–Wingdingsx] [Diabetologia (1994) 37: 745–749]

Notes: [Auszug] Young, low-mass stars are luminous X-ray sources whose powerful X-ray flares may exert a profound influence over the process of planet formation. The origin of the X-ray emission is uncertain. Although many (or perhaps most) recently formed, low-mass stars emit X-rays as a consequence of ...

Notes: Application criteria of steroid therapy for the patients of IgA nephropathy (IgAN) have not yet been established. The purpose of the present study was to establish retrospectively the clinical and pathological criteria for the steroid therapy by using a histological scoring on 104 adult patients of IgAN. Steroid therapy was designated as an administration of prednisolone in the amount of more than 30 mg per day in the period of more than 4 weeks within 1 year of kidney biopsy.We developed our own scoring system for the following main glomerular and tubulointerstitial changes as shown in 〈link href="#t1"〉Table 1. The histological scoring was expressed by evaluating semiquantitatively the extent of glomerular and tubulointerstitial lesions in terms of activity index (AI) and chronicity index (CI). Activity index is the sum of graded score according to the extent of glomeruli with mesangial hypercellularity, intracapillary macrophagic infiltration and cellular crescent as well as to the extent of interstitial inflammation and tubulitis. Chronicity index is the sum of graded score according to the extent of glomeruli with global sclerosis, increase of extracellular matrices or periglomerular fibrosis, and tuft adhesion or fibrous (or fibrocellular) crescent as well as to the extent of interstitial fibrosis (〈link href="#t1"〉Table 1).〈tabular xml:id="t1"〉1〈title type="main"〉 Histological scoring 〈table frame="topbot"〉〈tgroup cols="5" align="left"〉〈colspec colnum="1" colname="col1" align="left"/〉〈colspec colnum="2" colname="col2" align="center"/〉〈colspec colnum="3" colname="col3" align="center"/〉〈colspec colnum="4" colname="col4" align="center"/〉〈colspec colnum="5" colname="col5" align="center"/〉〈thead valign="bottom"〉〈row rowsep="1"〉Score0123〈tbody valign="top"〉〈entry namest="col1" nameend="col5" align="left"〉AI: Activity Index〈entry namest="col1" nameend="col5" align="left"〉G: glomerularm: mesangial hypercellularity−〈 40%〈 80%≥ 80%i: intracapillary macrophage infiltration−+++e: cellular crescent0〈 30%≥ 30%〈entry namest="col1" nameend="col5" align="left"〉I: tubulointerstitiali: interstitial inflammation−+++t: tubulitis−+++〈entry namest="col1" nameend="col5" align="left"〉CI: Chronicity Index〈entry namest="col1" nameend="col5" align="left"〉G: glomerulars: global sclerosis〈 10%〈 30%〈 50%≥ 50%i: increase of extracellular matrix〈 10%〈 30%〈 50%≥ 50%e: fibrous (or fibrocellular) crescent, adhesion〈 10%〈 30%〈 50%≥ 50% I: tubulointerstitial
 interstitial fibrosis〈 10%〈 30%〈 50%≥ 50%〈note xml:id="t1_note5" numbered="no"〉AI: AGm + AGi + AGe*2 + AIi + Ait, CI: CGS + CGi + CGe + CIFor the applicability of steroid therapy, three groups were categorized by evaluating the statistical significance for the correlation of AI, CI and daily amount of urine protein to the outcome of the patients as follows (〈link href="#t2"〉Table 2). In group A (inappropriate indication of steroid therapy) which showed CI ≥ 5 alone, 10 out of 11 cases revealed decline of renal function (Cr ≥ 1.2 mg/dL and Ccr 〈 80 mL/min) within 2.2–19.3 years (mean 9.0 ± 6.4 years) without respect to steroid therapy. In group B (unnecessary indication of steroid therapy) which showed CI 〈 5, AI 〈 5, and UP 〈 1 g/day, 58 out of 60 cases showed normal renal function (Cr 〈 1.2 mg/dL and Ccr ≥ 80 mL/min) within 4.2–21.6 years (mean 10.1 ± 4.7 years). In group C (necessary indication of steroid therapy) which showed CI 〈 5 and AI ≥ 5 or UP ≥ 1 g/day, patients with steroid therapy revealed significantly higher incidence of outcome with normal renal function (12 out of 13 patients, final evaluation of renal function in 6.8 ± 2.3 years after renal biopsy) than that of the patient without steroid therapy (seven out of 20 cases, evaluation of renal function in 9.2 ± 4.0 years after renal biopsy) (P 〈 0.01) (〈link href="#t3"〉Table 3). In the 13 patients with steroid therapy in group C (steroid pulse in four patients, prednisolone 40 mg/day internally in three patients, predonisolone 30 mg/day internally in six patients) showed a significant decrease of proteinuria and remained until final evaluation time (〈link href="#t4"〉Table 4).〈tabular xml:id="t2"〉2〈title type="main"〉 Application criteria of steroid therapy 〈mediaResource alt="image" href="urn:x-wiley:13205358:NEP15:NEP_15_t2"/〉〈tabular xml:id="t3"〉3〈title type="main"〉 Comparison of steroid (−) with steroid (+) in the group of ‘necessary’ 〈table frame="topbot"〉〈tgroup cols="4" align="left"〉〈colspec colnum="1" colname="col1" align="left"/〉〈colspec colnum="2" colname="col2" align="center"/〉〈colspec colnum="3" colname="col3" align="center"/〉〈colspec colnum="4" colname="col4" align="center"/〉〈thead valign="bottom"〉〈row rowsep="1"〉steroid therapy+− P 〈row rowsep="1"〉no.1320〈tbody valign="top"〉〈entry namest="col1" nameend="col4" align="left"〉At Renal Biopsyage (years)〈entry align="char" char="[plusmn]"〉31.5 ± 12.936.3 ± 13.0nsUP (g/day)〈entry align="char" char="[plusmn]"〉2.3 ± 1.91.3 ± 0.5〈 0.05Cr (mg/dL)〈entry align="char" char="[plusmn]"〉0.8 ± 0.30.9 ± 0.1nsCCr (mL/min)〈entry align="char" char="[plusmn]"〉111 ± 4392 ± 34nsHypertension (n)19ns+ ACEI (n)410nsFollow-up years from
 renal biopsy〈entry align="char" char="[plusmn]"〉6.8 ± 2.39.2 ± 4.0ns〈entry namest="col1" nameend="col4" align="left"〉End of follow-upCr (mg/dL)〈entry align="char" char="[plusmn]"〉0.8 ± 0.35.5 ± 6.6〈 0.01 Normal renal function
 (n)127 Renal insufficiency (n)16〈 0.01 Dialysis (n)07〈tabular xml:id="t4"〉4〈title type="main"〉 Change of urine protein in the 13 cases with steroid treatment in the group of 'necessary' 〈mediaResource alt="image" href="urn:x-wiley:13205358:NEP15:NEP_15_t4"/〉From the results above, our evaluation system using histological scoring together with grading proteinuria was proven to be useful in estimating the applicability of steroid therapy for adult IgAN patients.

Notes: Copper phtalocyanine (CuPc) films with the thickness controlled in molecular scales have been grown epitaxially on (0001) surfaces of layered materials, and electronic interaction at the interfaces have been studied by photoelectron spectroscopy. Materials with different electronic properties having different work functions (Evac) were chosen as the substrates; semiconducting MoTe2 (Evac=4.0 eV), semi-metallic highly oriented pyrolytic graphite (Evac=4.5 eV) and metallic TaSe2 (Evac=5.5 eV). Formation of interface dipole layers was found at CuPc/TaSe2 interfaces and molecular orbitals involved were identified. © 1998 American Institute of Physics.