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Ghassan Haddad*
Serhal Hospital, Lebanon
*Corresponding author: Ghassan Haddad, Serhal Hospital, Lebanon
Submission: July 04, 2018; Published: July 06, 2018
Advances in The Therapy of Depression
Editorial
Depression is one of the most common serious medical
and psychiatric disorders, with greater than 200 million adults
worldwide suffering from major depressive disorder (MDD) at
any given time, according to a 2003 report by the World Health
Organization titled Investing in Mental Health.
According to the U.S. National Comorbidity Survey Replication
published in 2007, more than 16 million adults in the United States,
which represents approximately 6.7% of itsentire adult population,
will suffer from MDD in a 12-month period.
The quest to come up with a superior antidepressant is in full
effectamongbiotechandpharmaceuticalcompanies.Althoughthere
are some companies that are still tweaking various formulations
of serotonergic, noradrenergic, and dopaminergic substances i.e.
triple reuptake inhibitors others are thinking outside the box.
Based on current research, the next decade of antidepressant
development will likely be drugs that affect the opioid receptors –
specifically the kappa receptor (OPKR).
OPKR and their endogenous neuropeptide ligand, dynorphin
A, are densely localized in limbic and cortical areas comprising the
brain reward system and are both upregulated by stress.
Researchers have discovered that developing opioid receptor
kappa (OPKR) antagonists may work extremely well for the
treatment of major depression. OPKR provides an antidepressant
response without significantly increasing pleasure (as would be
derived from stimulation of the opioid mu receptors(Figure 1).
Editorial
1/2Copyright © All rights are reserved by Ghassan Haddad.
Volume 2 - Issue - 1
Figure 1.
Techniques in
Neurosurgery & NeurologyC CRIMSON PUBLISHERS
Wings to the Research
ISSN 2637-7748
Tech Neurosurg Neurol Copyright © Ghassan Haddad
2/2
Volume 2 - Issue - 1
How to cite this article: Ghassan H.Advances in The Therapy of Depression. Tech Neurosurg Neurol. 2(1). TNN.000526.2018.
DOI: 10.31031/TNN.2018.02.000526
New Kappa Opioid Receptor Antagonists for Depression:
A. ALKS-5461
Of all kappa-receptor antagonists in development, this is
perhaps the most exciting. It combines a drug that alleviates
depression (Buprenorphine) with another drug (Samidorphan)
which negates any significant pleasure response by selective
antagonism of the mu-receptor. The early stages of clinical trials are
promising, so much so that the FDA granted it fast track designation.
Many people with depression find that antidepressants alone are
unable to adequately address all of their symptoms especially the
depressed mood and lack of energy, the FORWARD-4 Study is set to
address that, and result will soon be released.
LY-2456302
This is a new antidepressant in development by the company Eli
Lily. They are developing a new kappa-opioid receptor antagonist
drug with short-acting properties to serve as an adjunctive
treatment for refractory forms of depression. Currently the drug
is in Phase II clinical trials in the United States.LY-2456302 has
been shown to elicit synergistic effects when combined with other
antidepressants (e.g.SSRI and TCAs).
LY-2456302 now called CERC-501 is currently being
evaluated by researchers at the Massachusetts General Hospital in
Collaboration with the National Institute of Mental Health (NIMH)
as an adjunct treatment option for those with “treatment-resistant”
forms of depression.
This gives a patient the best-case scenario: an opioid-based
antidepressant response without a risk of dependency.Another
clinical trial is currently assessing the OPKR in mood and anxiety.
The study is called FASTMAS (Fast-Fail Trials in Mood and Anxiety
Spectrum Disorders.
Before the development of antidepressants, opioid agonists
were used to treat depression. This practice was consistent with
recent findings of depression-related dysregulation of the opioid
receptor and with mood improvement in treatment-resistant
depression after treatment with the mixed agonist/antagonist
buprenorphine.
A current placebo-controlled study involving 32 depressed
subjects who had failed a single antidepressant trial, researchers
tested a medication combining an opioid agonist (buprenorphine,
8 mg) with an opioid antagonist (samidorphin). Compared with
placebo, treatment at 1 week was associated with significantly
greaterandfasterreductionsinscoresonastandardizeddepression
rating scale and minimally increased euphoria scores. The active
treatment was associated with mild dizziness and nausea.
CERC-501 will be available as monotherapy or adjuvant therapy
with other first-line antidepressants in the treatment of Treatment
resistant depression, if ongoing clinical trials continue to provide
positive benefit-risk profiles.
Individuals that have taken Suboxon (an opioid replacement
drug) know that it works pretty well at eliciting an antidepressant
response. In fact, it tends to work so well that individuals who are
classified as having treatment-resistant depression often are able
to get significant relief with Suboxone. From a medical perspective,
the major problem with using Suboxone to treat depression is that
it affects the mu-opioid receptor, resulting in pleasurable effects
and potential dependency.
The STAR-D Report, 51.4% of patients failed to respond,
defined as achieving a 50% reduction in symptoms, and only 36.8%
became symptom free, or achieved remission, after their initial 12-
week. New extensive researches might bring more drug candidates
targeting the endogenous opioid system to clinical trials to address
current challenges in MDD treatment in clinical practice.For suicidal
patients and for patients with treatment resistant depression OPKR
antagonists brings new hope.
For possible submissions Click Here Submit Article
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Techniques in Neurosurgery & Neurology
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Advances in The Therapy of Depression_Crimson Publishers

  • 1. Ghassan Haddad* Serhal Hospital, Lebanon *Corresponding author: Ghassan Haddad, Serhal Hospital, Lebanon Submission: July 04, 2018; Published: July 06, 2018 Advances in The Therapy of Depression Editorial Depression is one of the most common serious medical and psychiatric disorders, with greater than 200 million adults worldwide suffering from major depressive disorder (MDD) at any given time, according to a 2003 report by the World Health Organization titled Investing in Mental Health. According to the U.S. National Comorbidity Survey Replication published in 2007, more than 16 million adults in the United States, which represents approximately 6.7% of itsentire adult population, will suffer from MDD in a 12-month period. The quest to come up with a superior antidepressant is in full effectamongbiotechandpharmaceuticalcompanies.Althoughthere are some companies that are still tweaking various formulations of serotonergic, noradrenergic, and dopaminergic substances i.e. triple reuptake inhibitors others are thinking outside the box. Based on current research, the next decade of antidepressant development will likely be drugs that affect the opioid receptors – specifically the kappa receptor (OPKR). OPKR and their endogenous neuropeptide ligand, dynorphin A, are densely localized in limbic and cortical areas comprising the brain reward system and are both upregulated by stress. Researchers have discovered that developing opioid receptor kappa (OPKR) antagonists may work extremely well for the treatment of major depression. OPKR provides an antidepressant response without significantly increasing pleasure (as would be derived from stimulation of the opioid mu receptors(Figure 1). Editorial 1/2Copyright © All rights are reserved by Ghassan Haddad. Volume 2 - Issue - 1 Figure 1. Techniques in Neurosurgery & NeurologyC CRIMSON PUBLISHERS Wings to the Research ISSN 2637-7748
  • 2. Tech Neurosurg Neurol Copyright © Ghassan Haddad 2/2 Volume 2 - Issue - 1 How to cite this article: Ghassan H.Advances in The Therapy of Depression. Tech Neurosurg Neurol. 2(1). TNN.000526.2018. DOI: 10.31031/TNN.2018.02.000526 New Kappa Opioid Receptor Antagonists for Depression: A. ALKS-5461 Of all kappa-receptor antagonists in development, this is perhaps the most exciting. It combines a drug that alleviates depression (Buprenorphine) with another drug (Samidorphan) which negates any significant pleasure response by selective antagonism of the mu-receptor. The early stages of clinical trials are promising, so much so that the FDA granted it fast track designation. Many people with depression find that antidepressants alone are unable to adequately address all of their symptoms especially the depressed mood and lack of energy, the FORWARD-4 Study is set to address that, and result will soon be released. LY-2456302 This is a new antidepressant in development by the company Eli Lily. They are developing a new kappa-opioid receptor antagonist drug with short-acting properties to serve as an adjunctive treatment for refractory forms of depression. Currently the drug is in Phase II clinical trials in the United States.LY-2456302 has been shown to elicit synergistic effects when combined with other antidepressants (e.g.SSRI and TCAs). LY-2456302 now called CERC-501 is currently being evaluated by researchers at the Massachusetts General Hospital in Collaboration with the National Institute of Mental Health (NIMH) as an adjunct treatment option for those with “treatment-resistant” forms of depression. This gives a patient the best-case scenario: an opioid-based antidepressant response without a risk of dependency.Another clinical trial is currently assessing the OPKR in mood and anxiety. The study is called FASTMAS (Fast-Fail Trials in Mood and Anxiety Spectrum Disorders. Before the development of antidepressants, opioid agonists were used to treat depression. This practice was consistent with recent findings of depression-related dysregulation of the opioid receptor and with mood improvement in treatment-resistant depression after treatment with the mixed agonist/antagonist buprenorphine. A current placebo-controlled study involving 32 depressed subjects who had failed a single antidepressant trial, researchers tested a medication combining an opioid agonist (buprenorphine, 8 mg) with an opioid antagonist (samidorphin). Compared with placebo, treatment at 1 week was associated with significantly greaterandfasterreductionsinscoresonastandardizeddepression rating scale and minimally increased euphoria scores. The active treatment was associated with mild dizziness and nausea. CERC-501 will be available as monotherapy or adjuvant therapy with other first-line antidepressants in the treatment of Treatment resistant depression, if ongoing clinical trials continue to provide positive benefit-risk profiles. Individuals that have taken Suboxon (an opioid replacement drug) know that it works pretty well at eliciting an antidepressant response. In fact, it tends to work so well that individuals who are classified as having treatment-resistant depression often are able to get significant relief with Suboxone. From a medical perspective, the major problem with using Suboxone to treat depression is that it affects the mu-opioid receptor, resulting in pleasurable effects and potential dependency. The STAR-D Report, 51.4% of patients failed to respond, defined as achieving a 50% reduction in symptoms, and only 36.8% became symptom free, or achieved remission, after their initial 12- week. New extensive researches might bring more drug candidates targeting the endogenous opioid system to clinical trials to address current challenges in MDD treatment in clinical practice.For suicidal patients and for patients with treatment resistant depression OPKR antagonists brings new hope. For possible submissions Click Here Submit Article Creative Commons Attribution 4.0 International License Techniques in Neurosurgery & Neurology Benefits of Publishing with us • High-level peer review and editorial services • Freely accessible online immediately upon publication • Authors retain the copyright to their work • Licensing it under a Creative Commons license • Visibility through different online platforms