srasi2018 Emerging sickle call agents target new pathways | Hematology News
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Emerging sickle cell agents target new pathways
Publish date: November 21, 2017
By Richard Mark Kirkner; Hematology News
1S FROM A M)
CONCORD, N.!
Approved treatments for sickle cell disease have been extremely limited, but
there are several therapies in the research pipeline that use new pathways to target the disease
“We do have much better understanding of the pathophysiology, which is getting us a few more
targets to aim at,” Julie Kanter, MD , director of sickle cell research at the Medical University of South Carolina,
Charleston, said at Sickle Cell Disease Symposium held by Carolinas Health Care System. These
targets include influencing how cells interact with the vascular endothelium, inhibiting
platelets, and preventing cell sickling and inflammation.
Dr. Julie Kanter
Earlier this year, the Food and Drug Administration approved L-glutamine oral powder
(Endari), although it is not yet widely available. This is only the second drug approved by the
FDA to treat sickle cell disease (SCD) and it’s the first approval in almost two decades. This
anti-inflammatory amino acid is indicated to reduce sickle cell crises. Dr. Kanter noted that a
48-week phase III trial demonstrated that L-glutamine reduced the frequency of sickle cell
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said Sounds Good
SCD pipeline
Deeper in the sickle cell pipeline is a class of antisickling agents known as hemoglobin
modifiers. “We're tying to change the way hemoglobin binds to oxygen, and if we can keep
hemoglobin binding to oxygen longer, it actually decreases the risk of hemoglobin sickling and
polymerizing in the cell,” Dr. Kanter explained.
One hemoglobin modifier is voxelotor (previously called GBT440), a once-daily oral agent that Global Blood Therapeutics
has in development
Another category of antisickling agents that researchers are looking at is anti-inflammatory
moderators, Dr. Kanter said. These include nitric oxide donors like sildenafil, which did not
“quite work” in SCD, and arginine and glutamine, which increase the amount of nitric oxide
once in the body “and hopefully reduce the risk of sickling,” she said. “If we can improve
inflammation, we might be able to improve the risk of cris
Cell adhesion modifiers are a drug class that aims to prevent cells from binding to each other.
These include platelet inhibitors and endothelial blockers. “There are several antiplatelet agents
that are approved really for stroke prevention or heart attack prevention, and we're trying to see
if we can repurpose these in sickle cell disease in a specific pathway that allows the platelet to
stick to the endothelium, but if we only inhibit one pathway it should not increase the risk of
bleeding,” Dr. Kanter said.
One platelet inhibition pathway that researchers are focused on is the P2Y,, adenosine
diphosphate blockade, which the platelet inhibitor prasugrel (Effient) acts on. A 2016 study of
this pathway in SCD “wasn’t successful,” Dr. Kanter said, “but it had some interesting results” ~
namely that the drug may be most effective in adolescents (N Engl J Med. 2016 Feb
18:374[7]:625-35 ).
Selectin-blocking medications are a drug class that act on white blood cell adhesion to, and
movement through, the endothelium, Dr. Kanter said. “Neutrophils can instigate a sickle cell
crisis, so if we can interrupt some of this rolling or sticking, could we decrease the risk of a
sickle cell crisis?” The drug GMI-1070 is currently being studied in a phase III trial and so far
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SUSTAIN trial, which included a cohort that also was taking hydroxyurea. T sounds Good 3
dose crizanlizumab resulted in an annual rate of that was more
le cell-related pain cri
than 45% lower than with placebo (N Engl J Med. 2017 Feb 2;376(5]:429-39
).
Stem cell transplants
Besides drugs, stem cell transplants to treat SCD have advanced in recent years to the point
where cure rates are exceeding 90%, Dr. Kanter noted. “However, the real issue with stem cells
is that patients still don’t have enough donors,” she said.
SCD is also potentially amenable to gene therapy, Dr. Kanter said, noting that SCD gene therapy
trials in progress are looking at harvesting patients’ own bone marrow, using the lentivirus viral
vector, inserting a gene to increase production of nonsickle hemoglobin, and using
myeloablative chemotherapy to remove old marrow and replace it with new, manipulated bone
marrow.
Several programs are investigating using a gene editing technique, known as CRISPR/Casg, to
alter the BCL11A gene to maintain fetal hemoglobin production.
“We all make fetal hemoglobin at birth, and then over 6 months to 1 year of life, our bodies
convert fetal hemoglobin to adult hemoglobin,” she said. “In sickle cell disease, it converts to
sickle hemoglobin. What if we could prevent that conversion and keep the fetal hemoglobin
turned on?” That could potentially eradicate the complications of SCD starting at an early age,
Dr. Kanter said.
Dr. Kanter, who has been involved in several of the SCD trials, reported relationships with
Pfizer, AstraZeneca, Bluebird Bio, Global Blood Therapeutics, Novartis, Guidepoint, GLG,
ApoPharma, and Purdue Pharma.
See LR Rake)
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