Cellular prion protein (PrPC) protects neuronal cells from the effect of huntingtin aggregation

Lee, Kyung Jin; Panzera, Antony; Rogawski, David; Greene, Lois E.; Eisenberg, Evan

doi:10.1242/jcs.004598

Cited by 24 publications

(14 citation statements)

References 49 publications

(52 reference statements)

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“…Crosstalk between PrP and other neurodegenerative disease causing proteins is not limited to AD, as another report has suggested that PrP protects against polyglutamine aggregate toxicity. 40 Tau, our study there was not a significant progressive rotarod deficit in α-synuclein Tg + mice or that the repeated testing had a masking effect on this phenotype ( Fig. 2A).…”

Section: Resultsmentioning

confidence: 46%

Context dependent neuroprotective properties of prion protein (PrP)

Steele

Zhou

Jackson

et al. 2009

Prion

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Section: Resultsmentioning

confidence: 46%

Context dependent neuroprotective properties of prion protein (PrP)

Steele

Zhou

Jackson

et al. 2009

Prion

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“…Plasmids encoding V5-tagged hNaa15p, hNaa25p, and hNaa35p were previously described (4,39,40). Plasmids encoding Huntingtin polyQ-enhanced green fluorescent protein (EGFP) fusion proteins (pHttQ25-EGFP, pHttQ72-EGFP, and pHttQ103-EGFP) (24,46) were generously provided by Evan Eisenberg, National Heart, Lung and Blood Institute, Bethesda, MD. Plasmids encoding EGFP-Huntingtin polyQ fusion proteins (pEGFP-HttQ23 and pEGFP-HttQ74) (45) were generously provided by David C. Rubinsztein, University of Cambridge, United Kingdom.…”

Section: Methodsmentioning

confidence: 99%

The Chaperone-Like Protein HYPK Acts Together with NatA in Cotranslational N-Terminal Acetylation and Prevention of Huntingtin Aggregation

Arnesen

Starheim

Damme

et al. 2010

Molecular and Cellular Biology

117

128

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The human NatA protein N ␣ -terminal-acetyltransferase complex is responsible for cotranslational Nterminal acetylation of proteins with Ser, Ala, Thr, Gly, and Val N termini. The NatA complex is composed of the catalytic subunit hNaa10p (hArd1) and the auxiliary subunit hNaa15p (hNat1/NATH). Using immunoprecipitation coupled with mass spectrometry, we identified endogenous HYPK, a Huntingtin (Htt)-interacting protein, as a novel stable interactor of NatA. HYPK has chaperone-like properties preventing Htt aggregation. HYPK, hNaa10p, and hNaa15p were associated with polysome fractions, indicating a function of HYPK associated with the NatA complex during protein translation. Knockdown of both hNAA10 and hNAA15 decreased HYPK protein levels, possibly indicating that NatA is required for the stability of HYPK. The biological importance of HYPK was evident from HYPK-knockdown HeLa cells displaying apoptosis and cell cycle arrest in the G 0 /G 1 phase. Knockdown of HYPK or hNAA10 resulted in increased aggregation of an Htt-enhanced green fluorescent protein (Htt-EGFP) fusion with expanded polyglutamine stretches, suggesting that both HYPK and NatA prevent Htt aggregation. Furthermore, we demonstrated that HYPK is required for N-terminal acetylation of the known in vivo NatA substrate protein PCNP. Taken together, the data indicate that the physical interaction between HYPK and NatA seems to be of functional importance both for Htt aggregation and for N-terminal acetylation.

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“…While suggested roles for PrP C include cell signaling, differentiation and adhesion, an increasing number of studies have implicated PrP C in neuroprotection against oxidative stress, ischemia and toxic protein aggregation. [27][28][29][30][31][32][33][34][35][36]38,46 Given the proposed neuroprotective role for PrP C , low levels of PrP C in CSF following spinal cord injury may well create a window in which neurons are susceptible to damage. CSF reduction in PrP C following spinal cord injury is specific (Figs.…”

Section: Discussionmentioning

confidence: 99%

“…Under normal conditions PrP C is released from cells into the CSF. [22][23][24][25][26] We evaluated PrP C in CSF samples for two reasons: First, PrP C has been hypothesized to be neuroprotective [27][28][29][30][31][32][33][34][35][36][37][38] and it follows that changes in CSF PrP C expression levels might influence neural cell survival. Secondly, CSF from some CJD patients is infectious 39 and changes in the CSF levels of PrP C may well alter the rate of PrP Sc replication.…”

mentioning

confidence: 99%