Rui Xue Wang scite author profile

Rui Xue Wang

5Publications

92Citation Statements Received

37Citation Statements Given

How they've been cited

123

How they cite others

153

Affiliations

Jinling Institute of Technology, University of North Carolina at Chapel Hill, Capital Normal University

Publications

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Gene Expression from the ORF50/K8 Region of Kaposi's Sarcoma-Associated Herpesvirus

Seaman

Wang

et al. 1999

Virology

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The ORF50 gene of Kaposi's sarcoma (KS)-associated herpesvirus, or human herpesvirus 8 (KSHV), activates viral replication and is weakly homologous to the herpesvirus family of R transactivators; therefore, the transcription and translation events from this region of KSHV are key events in viral reactivation. We demonstrate that ORF50 is expressed in a bicistronic message after induction of the viral lytic cycle. ORF50 migrated as a series of polypeptides: the major ones as 119 and 101 kDa, respectively. Using 3' rapid amplification of cDNA ends, RT-PCR, and cDNA library screening, we demonstrate that the major ORF50 transcript also encodes K8. The ORF50/K8 transcript was resistant to cyclohexamide, whereas the K8 transcript was only partially resistant to cyclohexamide at early timepoints. Both transcripts showed partial resistance after 12 h of phorbol ester induction. Using a GAL4-ORF50 fusion protein expression vector, we demonstrate that the transactivation domain of ORF50 resides within a 160-amino-acid region of the carboxyl portion of the ORF. Upstream regions of both ORF50 and K8 have basal promoter activity in KSHV-infected cells. K8, which had sequence homology to Bzip proteins, did not activate either promoter. However, both promoters were activated after cotransfection of ORF50 in BCBL-1 cells.

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An assessment of the genomics, comparative genomics and cellulose degradation potential of Mucilaginibacter polytrichastri strain RG4-7

Wang

Zhou

et al. 2020

Bioresource Technology

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Longitudinal sero‐reactivity to human herpesvirus 8 (KSHV) in the Swiss HIV Cohort 4.7 years before KS

Quinlivan

Wang

Stewart

et al. 2001

Journal of Medical Virology

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The relationship between viral infection with Kaposi sarcoma-associated herpesvirus (KSHV) and the onset of Kaposi sarcoma (KS) in AIDS patients is incompletely understood. This study investigates the use of three serological assays to predict the development of KS in HIV-positive patients. Serially collected serum samples from 36 patients with KS and matched controls in the Swiss HIV Cohort Study (SHCS) were analyzed in a case control study. Three serologic assays to detect antibodies against KSHV (nuclear and membrane antigen immunofluorescence assay, N-IFA, M-IFA and ORF 65.2 ELISA) were used to determine the predictive value of KSHV-seropositivity. Serial samples from the cases were also analyzed to determine longitudinal patterns of seroreactivity and identify cases of seroconversion. Assay sensitivity for detection of KSHV antibodies was highest for M-IFA (83%), followed by N-IFA (74%) and 65.2 ELISA (52%). At the time of initial serum sampling (median 4.7 years before KS), only the N-IFA distinguished case and control sera (61% vs. 32%) and no assay was clearly predictive of subsequent onset of clinical KS. Moreover, an unexpectedly high rate of reversions to seronegativity were observed by N-IFA (27/33) as well as by 65.2 ELISA (11/26) in the longitudinal analysis. Analysis of the ORF65.2 ELISA index indicated that these reversions before the clinical onset of KS were associated with antibody levels that frequently hovered around the level of detectability. A marked increase in ORF 65.2 antibody titer occurred in a third of the patients at the time of KS diagnosis. Only two seroconversions were documented. KSHV infection within the SHCS is likely to have preceded HIV infection. KSHV infection alone is not highly predictive of KS development in this cohort of HIV-infected homosexual men as compared with matched controls. Three KSHV serologic assays, though sensitive at the time of clinical KS are inconsistently positive before the development of AIDS-related KS.

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Laser Ablation in Liquid Synthesis and Optical Temperature Sensing of YGdO<sub>3</sub>:Er<sup>3+</sup> Nanoparticles

Liu

Wang

Chen³

2021

MSF

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YGdO3:Er3+ nanoparticles were successfully synthesized by pulsed laser ablation in liquid method. The structural and morphological properties of the product are investigated by X-Ray diffraction and transmission electron microscopy. The upconversion photoluminescence properties were investigated in detail. Obvious stark splitting phenomena were observed in the green and red emission bands. The decay behaviors of three emission bands were studied. Based on thermal coupled energy level related upconversion fluorescence intensity ratio, the temperature sensing properties of product were studied. Linear function has beenused to reveal the relationship between fluorescence intensity ratio and temperature. Using stark sublevels related emission bands, sensitivity of the temperature sensor was successfully enhanced. These results suggest the YGdO3:Er3+ nanoparticles prepared via pulsed laser ablation in liquid are promising luminescent materials for optical thermometry.

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Gene Expression from the ORF50/K8 Region of Kaposi's Sarcoma-Associated Herpesvirus

Seaman¹,

Ye²,

Wang³

et al. 1999

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Rui Xue Wang

Gene Expression from the ORF50/K8 Region of Kaposi's Sarcoma-Associated Herpesvirus

An assessment of the genomics, comparative genomics and cellulose degradation potential of Mucilaginibacter polytrichastri strain RG4-7

Longitudinal sero‐reactivity to human herpesvirus 8 (KSHV) in the Swiss HIV Cohort 4.7 years before KS

Laser Ablation in Liquid Synthesis and Optical Temperature Sensing of YGdO<sub>3</sub>:Er<sup>3+</sup> Nanoparticles

Gene Expression from the ORF50/K8 Region of Kaposi's Sarcoma-Associated Herpesvirus

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