Lymphoma Clinical Trial
Official title:
A Study of the Selective HDAC6 Inhibitor, ACY-1215, for the Treatment of Patients With Relapsed or Refractory Lymphoid Malignancies
This will be an open-label, single agent, multi-institutional phase Ib/II study of ACY-1215
for the treatment of patients with relapsed or refractory lymphoid malignancies. The target
population will include patients with histologically confirmed relapsed or refractory
non-Hodgkin's lymphoma or Hodgkin's lymphoma, with an expansion cohort of patients with
mantle cell lymphoma.
The phase Ib will be conducted to determine the safety and tolerability of two dosing
schedules of ACY-1215 monotherapy in patients with lymphoid malignancies. Patients will be
accrued simultaneously to two dose cohorts (Arm A and Arm B) of ACY-1215. Selection into each
cohort will occur by alternation. All patients will take the prescribed dose of ACY-1215
orally for 28 consecutive days. Patients enrolled into Arm A will take ACY-1215 160 mg daily
(QD), whereas patients enrolled into Arm B will take ACY-1215 160 mg twice daily (BID).
ACY-1215 will be supplied as a liquid for oral administration (PO). Each dose will be
administered at least 1 hour after ingestion of food followed by at least 4 ounces of water.
Patients will be instructed not to ingest food or other oral medication for at least 2 hours
after each ACY-1215 dose. Frequency in phase II will be determined based on Phase Ib results.
The emergence of epigenetic therapies has identified pan-class deacetylase (DAC) inhibitors
as effective therapeutic agents for the treatment of lymphoma. While pan-class DAC inhibitors
have led to FDA indications, clinical activity has been limited to the T-cell derived
malignancies. The mechanism of action remains largely unknown and off-target effects lead to
side effects including fatigue, gastrointestinal disturbances, and cytopenias. Recently, the
development of isoform selective DAC inhibitors have opened the opportunity to investigate
their mechanism. It is now recognized that DAC inhibitors not only have epigenetic
properties, but have direct effects on transcription factors (p53), oncogenes (Bcl6), and
protein degradation pathways (aggresome). Proteolysis occurs primarily through the
ubiquitin-proteosome pathway. In states where this pathway is physiologically overwhelmed or
therapeutically inhibited, the aggresome sequesters proteins for degradation. DAC6 is a class
IIb deacetylase that facilitates misfolded protein transport to the aggresome for
proteosome-independent proteolysis. Inhibition of the aggresome activates the unfolded
protein response (UPR) pathway, a cellular quality control mechanism with two primary
functions: (1) to promote survival during cellular endoplasmic reticulum (ER) stress by
chaperoning proteins back for re-folding and halting further transcription until homeostasis
is restored and (2) to signal CCAAT/enhancer binding protein (C/EBP)-homologous protein
(CHOP) mediated apoptosis when homeostasis cannot be reestablished[9]. While most cells
depend on both branches of the UPR to coordinate protein folding, lymphocytes physiologically
down-regulate the UPR-apoptosis pathway, specifically CHOP, to allow for generation of high
affinity antibodies. In addition to initiating genetic abnormalities (translocations and
point mutations) lymphomas inherit this biology, and thus gain a survival advantage.
It has been shown ACY-1215, an Histone Deacetylase 6 (HDAC6)-selective, orally active
small-molecule enzyme inhibitor has had single agent activity in a panel of lymphoma cell
lines and mouse models, and marked synergistic activity with several agents such as
bortezomib, carfilzomib, and ibrutinib, unpublished data. ACY-1215 has been studied in vivo
in models of multiple myeloma and lymphoma with marked activity both as a single agent and in
combination with bortezomib. Therefore ACY-1215 will be investigated for treatment of
lymphoma as a single agent leading to future studies evaluating its effects in combination
with other targeted agents known to be active in lymphoma and synergistic with ACY-1215.
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