RESUMEN
Phytophthora rot caused by Phytophthora sojae is a common and significant disease of soybean (Glycine max) in Illinois and throughout the Midwestern United States. The pathogenic characteristics of P. sojae populations in several Midwestern states have been reported recently, but pathogenicity and fungicide sensitivity traits of populations in Illinois were poorly understood. Isolates (n = 121) of soybean-infecting Phytophthora spp. were baited using susceptible cv. Sloan seedlings from soybean field soils with a history of seedling diseases in 24 counties across Illinois. The pathotype and race of isolates of P. sojae were characterized using 11 differential soybean cultivars in greenhouse tests using a hypocotyl inoculation method. Sensitivity to the fungicidal compounds metalaxyl and mefenoxam was tested with 63 isolates in vitro. Most (96%) of the Phytophthora isolates sampled from Illinois soybean fields were P. sojae, but 4% were an unidentified Phytophthora sp. as determined by phenotypic and genotypic traits. We present a preliminary description of another Phytophthora sp. from soybean fields in a restricted region of Illinois that is pathogenic and capable of killing soybean. Based on eight Rps gene differentials (Rps1a, 1b, 1c, 1d, 1k, 3a, 6, and 7 ), 22 virulence pathotypes of P. sojae were identified and 88% of all isolates were characterized to a defined race. The four most common races, which were 58% of all isolates, were races 1 (21%), 4 (15%), 33 (12%), and 28 (10%). Based on 11 differentials, (those noted above and Rps 2, 4, and 5), 31 virulence pathotypes were identified. The mean virulence complexities, which are the number of susceptible interactions on the sets of 8 and 11 Rps gene differentials, were 3.3 and 3.7, respectively. All isolates tested were sensitive to Apron XL, Allegiance, technical grade mefenoxam, and technical grade metalaxyl at 1.0 µg a.i./ml. The population of P. sojae is diverse and composed of multiple pathotypes and races in Illinois, and the results suggest that pathogen virulence partially explains poor performance of Phytophthora-resistant cultivars in many Illinois soybean fields.
RESUMEN
N-Demethylated metabolites of the antineoplastic agent hexamethylmelamine were synthesized, and their toxicities and antitumor activities were determined in vivo. Determinations of the lethal dose for 10% of the male C57BL X DBA/2 F1 (hereafter called BD2F1) mice showed hexamethylmelamine toxicity to be decreased by N-demethylation; the metabolites showed a direct relationship between potency (mmoles/kg/day) and number of methyl groups present. In BD2F1 mice bearing Sarcoma 180 or Lewis lung carcinoma, the antitumor activities of the methylmelamines decreased with a reduction in number of methyl groups, but were similar at equitoxic levels. Results were similar in L1210 leukemic mice treated with lethal dose levels of the metabolites for 10% of the mice when mean survival times were measured. The therapeutic equality produced with equitoxic levels, together with the ineffectiveness of melamine, suggested that the presence of a methyl group, rather than the number, was the determining factor in the antitumor activity of the methylmelamines.
Asunto(s)
Altretamina/toxicidad , Altretamina/uso terapéutico , Neoplasias Experimentales/tratamiento farmacológico , Triazinas/toxicidad , Triazinas/uso terapéutico , Altretamina/metabolismo , Animales , Dosificación Letal Mediana , Leucemia L1210/tratamiento farmacológico , Neoplasias Pulmonares/tratamiento farmacológico , Masculino , Ratones , Ratones Endogámicos C57BL , Ratones Endogámicos DBA , Neoplasias Experimentales/mortalidad , Sarcoma 180/tratamiento farmacológico , Relación Estructura-ActividadRESUMEN
The addition of deoxyuridine (UDR) to fluorouracil (FU) or floxuridine (5-fluoro-2' deoxyuridine) (FUDR) produced a substantial increase in their toxicity in BDF1 mice. Antitumor assays using sarcoma 180 tumor-bearing mice showed a concomitant increase in tumor growth inhibition for the nucleoside-drug combination over identical doses of the single drug. However, no significant increase in antitumor activity with the combination treatment was demonstrated when equitoxic doses were given. Additional support for the therapeutic equality of the single and combination drug regimens was the similarity of the therapeutic indexes for each treatment regimen involving either fluorouracil or floxuridine. The results suggested that any therapeutic benefit achieved with the combination therapy could be duplicated with either fluorouracil or floxuridine at a higher dose.
