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Editorial
Interfering with epigenetics in hepatocellular carcinoma: Out of the shelter?
Chris Verslype,
doi:10.1016/j.jhep.2016.03.017
Refers To
Michael Bitzer, Marius Horger, Edoardo G. Giannini, Tom M. Ganten, Marcus A. Wörns, Jens T. Siveke, Matthias M. Dollinger, Guido Gerken, Max E. Scheulen, Henning Wege, Vittorina Zagonel, Umberto Cillo, Franco Trevisani, Armando Santoro, Vincenzo Montesarchio, Nisar P. Malek, Julia Holzapfel, Thomas Herz, Astrid S. Ammendola, Stefano Pegoraro, Bernhard Hauns, et al.
Resminostat plus sorafenib as second-line therapy of advanced hepatocellular carcinoma – The SHELTER study
Journal of Hepatology, Volume 65, Issue 2, August 2016, Pages 280-288
Histone deacetylases (HDACs) regulate gene expression by enzymatic removal of the acetyl group from histones, making the DNA more compact and as such, silencing genes. At least 18 HDACs are known, and although the name refers to a histone substrate, the activity of HDACs is not limited to histones. They act also as acetyl-lysin removers on a variety of non-histone proteins with diverse biological functions (e.g., transcription factors p53, NF-κB and many others) [1].
In several cancers, including hepatocellular carcinoma (HCC), overexpression of individual HDACs has been shown to correlate with poor prognosis [2]. HDAC3 overexpression in HCC was significantly correlated with advanced tumor stage and early recurrence of HCC after surgery [3]. Moreover, HDAC3 was found to be selectively expressed in liver cancer stem cells (CSCs) and implicated in self-renewal of liver CSCs [3]. In contrast, some HDACs may exert a tumor suppressor role as liver-specific knockdown of HDAC3 resulted in overt HCC [4]. Especially persistent inactivation of the HDAC3/NCOR/SMRT axis may be detrimental, promoting the development of cancer by allowing the increase of histone acetylation during the S phase, leading to DNA damage [4]. HDACs may therefore not only serve as therapeutic targets in advanced cancer, but also act as tumor suppressors in developing tumors [5]. Inhibiting HDAC may lead to disruption of many pathways and may complicate a rational drug design.
A large number of HDAC inhibitors (HDACis) are of natural origin and present in garlic (allyl mercaptan), blueberries (piceatannol), broccoli (sulforaphane) and grapes (reversatrol) [6]. So far, three pan-HDAC inhibitors have been approved for the therapy of refractory cutaneous and peripheral T cell lymphoma (somidepsin, vorinostat and belinostat) [7] and others are under investigation for hematologic and solid cancers. The mode of action of this class of drugs seems to be related to apoptosis induction in tumor cells. The most common toxicities of HDACis are bone marrow suppression, fatigue and diarrhea [5]. In solid tumors, monotherapy with these agents has yielded insufficient responses.
The only phase I/II clinical trial so far using the HDAC inhibitor belinostat in patients with advanced HCC (62% first-line treatment), reported a disappointing median progression free survival (PFS) and overall survival (OS) of 2.64 and 6.6 months respectively [8].
In this issue of the Journal of Hepatology, Bitzer et al. report the results of the SHELTER study, a phase I/II clinical trial of resminostat, belonging to the same hydroxamic acid class of HDACis as belinostat [9]. Patients with advanced HCC and documented progression under treatment with sorafenib, were treated with resminostat, either alone or in combination with sorafenib. The combination treatment provided a PFS of 6.5 months and an OS of 8.1 months. In contrast, the results for the monotherapy group treated with resminostat were very poor. There were no unexpected or problematic safety issues. At first sight, the 8 months OS for resminostat and sorafenib may not seem exceptional, and comparable to the outcome of patients in the placebo arms of recent second-line trials [10]. However, the SHELTER investigators exclusively studied patients with documented sorafenib progression (and not sorafenib intolerance). There were no imbalances in the pattern of progression prior to entry in the study, that has recently been shown to be of prognostic importance and only a minority of patients was in the most favorable group [11].
Despite the moderate benefit and the non-randomized small nature of the study, this trial may revitalize the interest in HDAC inhibitors for advanced HCC. Treatment of sorafenib (with escalating doses) beyond progression has been previously evaluated and yielded no benefit [12]. The finding that resminostat may restore sensitivity to sorafenib represents the most important message from this trial. A future first-line phase III study may test the upfront combination of sorafenib and resminostat, vs. the addition to sorafenib of the HDAC inhibitor at the time of progression. Such a trial may also investigate the value of the transcription factor ZFP64, which has been suggested as a prognostic and predictive factor by the investigators of the SHELTER study.
To date, no established regimens exist for the treatment of patients with advanced HCC after failure of first-line treatment with the multikinase inhibitor sorafenib. While awaiting the results of the current phase III studies with cabozantinib, tivantinib, regorafinib and the promise of immunotherapy, we may now also consider the restoration of sensitivity to sorafenib by resminostat as a potential therapeutic option.
Conflict of interest
C. Verslype received research funding from Bayer, Pfizer, Ipsen, Sirtex and Novartis.
References
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发表于 2016-7-16 20:44