Resveratrol Rescues SIRT1-Dependent Adult Stem Cell Decline and Alleviates Progeroid Features in Laminopathy-Based Progeria

Liu, Baohua; Ghosh, Shreya; Yang, Xi; Zheng, Heng; Liu, Xinguang; Wang, Zimei; Jin, Guoxiang; Zheng, Bo‐Jian; Kennedy, Brian K.; Suh, Yousin; Kaeberlein, Matt; Tryggvason, Karl; Zhou, Zhongjun

doi:10.1016/j.cmet.2012.11.007

Cited by 173 publications

(144 citation statements)

References 68 publications

Supporting

Mentioning

139

Contrasting

Unclassified

Order By: Relevance

“…This is in agreement with several previous reports (Borra et al 2005;Kaeberlein et al 2005;Beher et al 2009;Pacholec et al 2010;Liu et al 2012) and contrasts with some others (Dai et al 2010;Hubbard et al 2013). Significantly, the two native peptides used in our experiments all have an aromatic residue at the +1 position, and the PGC-1α peptide also contains an additional aromatic residue at the +6 position, which has been suggested to further stimulation of SIRT1 activity by STACs (Hubbard et al 2013).…”

Section: Discussioncontrasting

confidence: 49%

“…However, it is not unprecedented that an NTD of sirtuin harbors an allosteric activation mechanism toward native substrates. For example, binding of Sir4, principally through the NTD of Sir2, stimulates deacetylation of H4K16 by Sir2 (Tanny et al 2004;Hsu et al 2013), and binding by AROS and Lamin A, suggested via the NTD of SIRT1, potentiates the activity of SIRT1 toward p53 (Kim et al 2007;Liu et al 2012). Therefore, it is possible that, by modeling the protein-protein interaction effect with small molecules, allosteric activation of SIRT1 activation may be achieved.…”

Section: Discussionmentioning

confidence: 99%

“…The structural information obtained here may facilitate a computational search of such compounds. The structural property of SIRT1, together with further information on protein-protein interaction, should also benefit the understanding of new activation mechanisms of SIRT1 involving additional binding factors, such as Lamin A, which is reported to synergize with resveratrol to stimulate SIRT1 activity (Liu et al 2012). …”

Section: Discussionmentioning

confidence: 99%

See 2 more Smart Citations

Structural basis for allosteric, substrate-dependent stimulation of SIRT1 activity by resveratrol

et al. 2015

View full text Add to dashboard Cite

Sirtuins with an extended N-terminal domain (NTD), represented by yeast Sir2 and human SIRT1, harbor intrinsic mechanisms for regulation of their NAD-dependent deacetylase activities. Elucidation of the regulatory mechanisms is crucial for understanding the biological functions of sirtuins and development of potential therapeutics. In particular, SIRT1 has emerged as an attractive therapeutic target, and the search for SIRT1-activating compounds (STACs) has been actively pursued. However, the effectiveness of a class of reported STACs (represented by resveratrol) as direct SIRT1 activators is under debate due to the complication involving the use of fluorogenic substrates in in vitro assays. Future efforts of SIRT1-based therapeutics necessitate the dissection of the molecular mechanism of SIRT1 stimulation. We solved the structure of SIRT1 in complex with resveratrol and a 7-amino-4-methylcoumarin (AMC)-containing peptide. The structure reveals the presence of three resveratrol molecules, two of which mediate the interaction between the AMC peptide and the NTD of SIRT1. The two NTD-bound resveratrol molecules are principally responsible for promoting tighter binding between SIRT1 and the peptide and the stimulation of SIRT1 activity. The structural information provides valuable insights into regulation of SIRT1 activity and should benefit the development of authentic SIRT1 activators.

show abstract

Section: Discussioncontrasting

confidence: 49%

Section: Discussionmentioning

confidence: 99%

Section: Discussionmentioning

confidence: 99%

See 1 more Smart Citation

Structural basis for allosteric, substrate-dependent stimulation of SIRT1 activity by resveratrol

et al. 2015

View full text Add to dashboard Cite

show abstract

“…Furthermore, HDAC2 has been shown to suppress p21 expression in human hepatocellular carcinoma via its binding to an Sp1‐binding site (Noh et al, 2011). On the other hand, it has been demonstrated that lamin A/C establishes direct interactions with histone deacetylases including SIRT1 (Cenni et al, 2014; Liu et al, 2012), SIRT6 (Ghosh, Liu, Wang, Hao, & Zhou, 2015), and HDAC1 (Kubben et al, 2016), while lamin partners at the nuclear envelope such as emerin, BAF, and LAP2beta interact with HDAC3 (Demmerle, Koch, & Holaska, 2013) or HDAC2 (Tsai et al, 2015). Moreover, lamin A/C has been demonstrated to bind gene promoters or neighboring domains and this binding has been linked to distinct transcriptional outcomes (Lee, Welton, Smith, & Kennedy, 2009; Lund & Collas, 2013; Mattout et al, 2011).…”

Section: Introductionmentioning

confidence: 99%

Altered modulation of lamin A/C‐HDAC2 interaction and p21 expression during oxidative stress response in HGPS

Mattioli¹,

Andrenacci²,

Garofalo

et al. 2018

Aging Cell

View full text Add to dashboard Cite

Defects in stress response are main determinants of cellular senescence and organism aging. In fibroblasts from patients affected by Hutchinson–Gilford progeria, a severe LMNA‐linked syndrome associated with bone resorption, cardiovascular disorders, and premature aging, we found altered modulation of CDKN1A, encoding p21, upon oxidative stress induction, and accumulation of senescence markers during stress recovery. In this context, we unraveled a dynamic interaction of lamin A/C with HDAC2, an histone deacetylase that regulates CDKN1A expression. In control skin fibroblasts, lamin A/C is part of a protein complex including HDAC2 and its histone substrates; protein interaction is reduced at the onset of DNA damage response and recovered after completion of DNA repair. This interplay parallels modulation of p21 expression and global histone acetylation, and it is disrupted by LMNAmutations leading to progeroid phenotypes. In fact, HGPS cells show impaired lamin A/C‐HDAC2 interplay and accumulation of p21 upon stress recovery. Collectively, these results link altered physical interaction between lamin A/C and HDAC2 to cellular and organism aging. The lamin A/C‐HDAC2 complex may be a novel therapeutic target to slow down progression of progeria symptoms.

show abstract

“…Moreover, this regulatory pathway may be altered in human progeria and should be assessed in progeroid mouse models. In one such model, Zmpste24 −/− mice, a model for Hutchinson-Gilford progeria associated with mutations in A-type lamins, loss of SIRT1 function has already been noted in MSC populations [11]. SIRT6 was not assessed in that study; however, another recent study showed that A-type lamins are required for SIRT6 activation and support SIRT6-mediated DNA repair [12].…”

mentioning

confidence: 92%

SIRT6, oxidative stress, and aging

Liao

Kennedy

2016

Cell Res

View full text Add to dashboard Cite

Resveratrol Rescues SIRT1-Dependent Adult Stem Cell Decline and Alleviates Progeroid Features in Laminopathy-Based Progeria

Cited by 173 publications

References 68 publications

Structural basis for allosteric, substrate-dependent stimulation of SIRT1 activity by resveratrol

Structural basis for allosteric, substrate-dependent stimulation of SIRT1 activity by resveratrol

Altered modulation of lamin A/C‐HDAC2 interaction and p21 expression during oxidative stress response in HGPS

SIRT6, oxidative stress, and aging

Contact Info

Product

Resources

About