D S Vallari scite author profile

Objective-To investigate the possible interference with acute hepatitis B virus infection by coinfection with hepatitis C virus.Design-Analysis of stored sera collected for transfusion transmitted viruses study in 1970s.Setting 479-2465 IUl1) and biphasic in patients with combined acute infection (no value >380 IU/1; p=0 0025). Four coinfected recipients developed chronic hepatitis C virus infection. The fifth patient was followed for only four months.Conclusions-Acute coinfection with hepatitis C virus and hepatitis B virus inhibits hepatitis B virus infection in humans, and onset of hepatitis B may reduce the severity of hepatitis C virus infection but not frequency of chronicity. Alanine aminotransferase concentration showed a biphasic pattern in dual infection.

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Biosynthesis and degradation both contribute to the regulation of coenzyme A content in Escherichia coli

Vallari

Jackowski

1988

J Bacteriol

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Escherichia coli mutants [coaA16(Fr); Fr indicates feedback resistance] were isolated which possessed a pantothenate kinase activity that was refractory to feedback inhibition by coenzyme A (CoA). Strains harboring this mutation had CoA levels that were significantly elevated compared with strains containing the wild-type kinase and also overproduced both intra-and extracellular 4'-phosphopantetheine. The origin of 4'-phosphopantetheine was investigated by using strain SJ135 ( (1 g/liter). The concentration of tetracycline hydrochloride was 10 ,Ig/ml. Cell number was monitored during growth by using a Klett-Summerson colorimeter with a blue filter. The colorimeter was calibrated with strain SJ16 by determining the number of viable bacteria in the range of colorimeter readings encountered.Strain SJ135 was a derivative of strain UB1005 constructed to contain the A(aroP-aceEF) deletion from strain SJ7, the panD2 mutation from strain SJ16, and the panFII allele from strain DV14 (Table 1).

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Isolation and characterization of temperature-sensitive pantothenate kinase (coaA) mutants of Escherichia coli

Vallari

Rock

1987

J Bacteriol

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Escherichia coli mutants conditionally defective in the conversion of pantothenate to coenzyme A were isolated and characterized. The gene was designated coaA and localized between argEH and rpoB near min 90 of the chromosome. The coaAl5(Ts) mutation caused a temperature-sensitive growth phenotype and temperature-dependent inactivation of pantothenate kinase activity assayed both in vivo and in vitro. At 30°C, coaA15(Ts) extracts contained less than 20% of the wild-type pantothenate kinase activity; the kinase had near normal kinetic constants for the substrates ATP and pantothenate and was inhibited by coenzyme A to the same degree as the wild-type enzyme. These data define the coaA gene as the structural gene for pantothenate kinase.Coenzyme A (CoA) is synthesized by a series of reactions beginning with the phosphorylation of the vitamin pantothenic acid (1). In Escherichia coli, pantothenate kinase catalyzes the rate-controlling step in the pathway (9,10

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The Natural History of Infection with Hepatitis C Virus (HCV) in Chimpanzees: Comparison of Serologic Responses Measured with First- and Second- Generation Assays and Relationship to HCV Viremia

Farci

London²,

Wong³

et al. 1992

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The sensitivity of first- and second-generation tests for antibody to hepatitis C virus (HCV) and the relationship among the patterns of antibody response and HCV viremia were examined in serial serum samples from 6 chimpanzees experimentally infected with HCV and followed less than or equal to 3 years. HCV infection was transient in 4 chimpanzees and became chronic in 2. All chimpanzees developed antibodies to HCV detectable by second-generation assays, while only 5 of the 6 became positive by first-generation assay. Second-generation were consistently more sensitive than first-generation assays for the early diagnosis of primary HCV infection. The pattern observed with second-generation assays was not influenced by the outcome of HCV infection, since antibodies remained persistently detectable throughout follow-up regardless of whether viremia was transient or persistent. In contrast, the first-generation antibody response was variable: It usually disappeared after loss of viremia, whereas its presence paralleled HCV viremia in chimpanzees with chronic infection.

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Temporal relationships of hepatitis C virus RNA and antibody responses following experimental infection of chimpanzees

Beach

Meeks

Mimms

et al. 1992

Journal of Medical Virology

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Liver enzyme levels, viral RNA, and the immune response against both structural and nonstructural hepatitis C virus (HCV) proteins have been studied in experimentally infected chimpanzees in order to further understand the natural history of HCV infection. An ELISA for measuring both IgG and IgM responses to core (c22), 33c (NS3), and c100 (NS4) was employed. The IgG response rates were 5/8 for core, and 8/8 for both 33c and c100. Utilizing this antigen combination, at least one antibody response is measureable at, or within 3 weeks of, the major ALT peak. Although no individual antibody response is universally associated with initial detection of seroconversion, the combination of all three recombinant proteins measures seroconversion an average of 54 days earlier than with c100 alone, in 6/8 of the animals. IgM responses were measureable in 5/8 of the chimpanzees, were of shorter duration, and usually arose concomitantly with IgG responses. IgM appears to be a good indicator of primary infection since neither boosting nor recrudescence of disease during the chronic phase of disease elicited a secondary IgM response. Viral RNA can be measured 4-7 days (average = 9 days) postinfection with the period preceding the ALT peak being characterized by several PCR positive segments interrupted by periods in which no viral RNA can be measured. Following the ALT peak, chronically infected animals with recurring ALT elevations are generally PCR positive with intercedent PCR negative periods. Those animals that appear to have biochemically resolved disease generally have PCR negative profiles, although they still may periodically exhibit PCR positive sera. This indicates that with the recent advent of new screening techniques, a more stringent definition of HCV resolution will be required.

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D S Vallari

Effect of concurrent acute infection with hepatitis C virus on acute hepatitis B virus infection.

Biosynthesis and degradation both contribute to the regulation of coenzyme A content in Escherichia coli

Isolation and characterization of temperature-sensitive pantothenate kinase (coaA) mutants of Escherichia coli

The Natural History of Infection with Hepatitis C Virus (HCV) in Chimpanzees: Comparison of Serologic Responses Measured with First- and Second- Generation Assays and Relationship to HCV Viremia

Temporal relationships of hepatitis C virus RNA and antibody responses following experimental infection of chimpanzees

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