Instytut Podstawowych Problemów Techniki
Polskiej Akademii Nauk

Pracownicy

mgr inż. Adithya Pallepati

Zakład Biosystemów i Miękkiej Materii (ZBiMM)
doktorant
telefon: (+48) 22 826 12 81 wewn.: 411
pokój: 326
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Ostatnie publikacje
1.  Bartak M., Krahel W., Chodkowski M., Grel H., Walczak J., Pallepati A., Komorowski M., Cymerys J., ATPase Valosin-Containing Protein (VCP) Is Involved During the Replication and Egress of Sialodacryoadenitis Virus (SDAV) in Neurons, International Journal of Molecular Sciences, ISSN: 1422-0067, DOI: 10.3390/ijms252111633, Vol.25, No.21, pp.11633-1-23, 2024

Streszczenie:
Sialodacryoadenitis virus (SDAV) has been identified as the etiological agent responsible for the respiratory system and salivary gland infections in rats. The existing literature on SDAV infections is insufficient to address the topic adequately, particularly in relation to the central nervous system. In order to ascertain how SDAV gains access to neuronal cells and subsequently exits, our attention was focused on the small molecule valosin-containing protein (VCP), which is an ATPase. VCP is acknowledged for its function in the ubiquitin-mediated proteasomal degradation of proteins, including those of viral origin. To ascertain the potential influence of VCP on SDAV replication and egress, high-content screening was employed to determine the viral titer and protein content. Western blot analysis was employed to ascertain the relative expression of VCP. Real-time imaging of SDAV-infected cells and confocal imaging for qualitative morphological analysis were conducted. The Eeyarestatin I (EerI) inhibitor was employed to disrupt VCP involvement in the endoplasmic reticulum-associated protein degradation pathway (ERAD) in both pre- and post-incubation systems, with concentrations of 5 μM/mL and 25 μM/mL, respectively. We demonstrated for the first time that SDAV productively replicates in cultured primary neurons. VCP expression is markedly elevated during SDAV infection. The application of 5 μM/mL EerI in the post-treatment system yielded a statistically significant inhibition of the SDAV yield. It is likely that this modulates the efficacy of virion assembly by arresting viral proteins in the submembrane area.

Słowa kluczowe:
SDAV,VCP,primary neurons,virion assembly,ERAD,eeyarestatin I

Afiliacje autorów:
Bartak M. - inna afiliacja
Krahel W. - inna afiliacja
Chodkowski M. - inna afiliacja
Grel H. - inna afiliacja
Walczak J. - IPPT PAN
Pallepati A. - IPPT PAN
Komorowski M. - IPPT PAN
Cymerys J. - inna afiliacja
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