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Critical care medicine. 2019:47.DOI:

PROTOCOLIZED URINE SAMPLING REDUCES CAUTI RATES [Meeting Abstract]

Frontera, Jennier; Weisstuch, Joseph; Phillips, Michael; Radford, Martha; Sterling, Stephanie; Delorenzo, Karen; Saxena, Archana; Wang, Erwin
ISI:000498593400576
ISSN: 0090-3493
CID: 4227692
Chemical communications (Cambridge, England). 2009(27):4103-5.DOI: 10.1039/b903059j

DNAzyme catalytic beacon sensors that resist temperature-dependent variations

Nagraj, Nandini; Liu, Juewen; Sterling, Stephanie; Wu, Jenny; Lu, Yi
The temperature-dependent variability of a Pb2+-specific 8-17E DNAzyme catalytic beacon sensor has been addressed through the introduction of mismatches in the DNAzyme, and the resulting sensors resist temperature-dependent variations from 4 to 30 degrees C
PMCID:3401477
PMID: 19568647
ISSN: 1359-7345
CID: 110800
Current HIV/AIDS reports. 2009:6(2):51-52.DOI:

New goals for viral suppression in HIV treatment in even the most experienced of patients

Sterling S.A.; Aberg J.A.
EMBASE:2009205056
ISSN: 1548-3568
CID: 99001
Journal of virology. 2003:77(5):2832-42.DOI: 10.1128/jvi.77.5.2832-2842.2003

Quantitative role of the human papillomavirus type 16 E5 gene during the productive stage of the viral life cycle

Genther, Sybil M; Sterling, Stephanie; Duensing, Stefan; Munger, Karl; Sattler, Carol; Lambert, Paul F
Human papillomaviruses (HPVs) are small circular DNA viruses that cause warts. Infection with high-risk anogenital HPVs, such as HPV type 16 (HPV16), is associated with human cancers, specifically cervical cancer. The life cycle of HPVs is intimately tied to the differentiation status of the host epithelium and has two distinct stages: the nonproductive stage and the productive stage. In the nonproductive stage, which arises in the poorly differentiated basal epithelial compartment of a wart, the virus maintains itself as a low-copy-number nuclear plasmid. In the productive stage, which arises as the host cell undergoes terminal differentiation, viral DNA is amplified; the capsid genes, L1 and L2, are expressed; and progeny virions are produced. This stage of the viral life cycle relies on the ability of the virus to reprogram the differentiated cells to support DNA synthesis. Papillomaviruses encode multiple oncoproteins, E5, E6, and E7. In the present study, we analyze the role of one of these viral oncogenes, E5, in the viral life cycle. To assess the role of E5 in the HPV16 life cycle, we introduced wild-type (WT) or E5 mutant HPV16 genomes into NIKS, a keratinocyte cell line that supports the papillomavirus life cycle. By culturing these cells under conditions that allow them to remain undifferentiated, a state similar to that of basal epithelial cells, we determined that E5 does not play an essential role in the nonproductive stage of the HPV16 life cycle. To determine if E5 plays a role in the productive stage of the viral life cycle, we cultured keratinocyte populations in organotypic raft cultures, which promote the differentiation and stratification of epithelial cells. We found that cells harboring E5 mutant genomes displayed a quantitative reduction in the percentage of suprabasal cells undergoing DNA synthesis, compared to cells containing WT HPV16 DNA. This reduction in DNA synthesis, however, did not prevent amplification of viral DNA in the differentiated cellular compartment. Likewise, late viral gene expression and the perturbation of normal keratinocyte differentiation were retained in cells harboring E5 mutant genomes. These data demonstrate that E5 plays a subtle role during the productive stage of the HPV16 life cycle
PMCID:149772
PMID: 12584306
ISSN: 0022-538x
CID: 110787