Article Type : Research Article
Authors : Lunde Dadiane A, Lunde Dadon JDV, Bridgesson S, Deaths S and Trondheim S
Keywords : Substance abuse; Chemical compounds; Diagnosis for underlying conditions; Opioid's; Heroin; Cocaine; Drug manufacturer; ATMP and Vector Control Products; Vaccines
In this Research Article we explain the Medical
Dossier information collected through APC and Dossier Codification of diagnosis
of substance abuse. Using this tool, we have a collective data set where we can
treat and diagnose substance abuse disorders and addiction medicine protocols.
Here we focus on underlying conditions affecting the prognosis of substance
abuse and addiction medicine diagnostic criteria.
In
this Research Article we explain the Medical Dossier information collected
through APC and Dossier Codification of diagnosis of substance abuse. Using
this tool, we have a collective data set where we can treat and diagnose
substance abuse disorders and addiction medicine protocols. Here we focus on
underlying conditions affecting the prognosis of substance abuse and addiction
medicine diagnostic criteria. The GLP-1 functions show suppression in opioid
abuse such as heroin, fentanyl, and morphine. It appears in studies and case
reports that liraglutide reduced craving for opioids and RCT in individuals
with OUD. GLP-1R agonist medication used for addiction treatment and substance
abuse as an underlying condition. RCT (Randomized Controlled Trial) and Opiod
Use Disorder is (OUD). The primary focus of RCT in Vector Control Products
(vaccines) is to adhere to efficacy and safety in treatment interventions
across the globe. Advanced Therapeutic Medicinal Products are tested through
Pharmaceutical Trials for results in treating conditions and underlying
pre-existing conditions, we will elaborate here. (Figure 1) [1].
Chemical Compounding information and research is important for setting drugs under classification for Addiction Drug Treatment. Preparing a Diagnosis through Pharmacology and Drugs Chemical Compounding Data is a rationale method to release the drug into the environmental with supportive documentation. For GLP-1R agents we used the generic MeSH Name for Liraglutide is a lipopeptide that is an analogue of human GLP-1 in which the lysine residue at position 27 is replaced by arginine and a hexadecanoyl group attached to the remaining lysine via a glutamic acid spacer. Used as an adjunct to diet and exercise to improve glycaemic control in adults with type 2 diabetes mellitus. It has a role as a glucagon-like peptide-1 receptor agonist and a neuroprotective agent. It is a lipopeptide and a polypeptide. We distinguished the issue with Diabetes mellitus and the glycaemic control mechanisms to opioid, heroin, and cocaine drug abuse. The information will be retained in this study to show that controlling glycaemic index in a "body" assists in the Addiction Medicine diagnosis and treatment (Figure 2).
Figure 1: Addiction Medicine track outcomes of variety of Drug Abuse rituals, tools, and how affect one another.
Figure 2: GLP-1R is research studied chemical drug used in pharmaceuticals for Randomized Controlled Trials and for OUD (Opiod Used Disorder). (IUPHAR, 2012}.
Here
we index the trial data for the FDA approved Drug Classification:
In order:
· WIPO PATENTSCOPE
Patents are available for this
chemical structure:
Cas No. 204656-20-02 Molecular Weight
3200 g/mol
https://patentscope.wipo.int/search/en/result.jsf?inchikey=YSDQQAXHVYUZIW-QCIJIYAXSA-N
· FDA Orange Book Patents
1 US Patent Trade AIPLA Name:
Liraglutide Application Number: (ECHA) 810-818-7per g/Mol= 3200-3800 g/mol
9968659*PED
SAXENDA
206321
· PubChem CID
16134956
Structure and Bioassay Data
· IUPAC Condensed
H-His-Ala-Glu-Gly-Thr-Phe-Thr-Ser-Asp-Val-Ser-Ser-Tyr-Leu-Glu-Gly-Gln-Ala-Ala-Lys(1)-Glu-Phe-lle-Ala-Trp-Leu-Val-Arg-Gly-Arg-Gly-OH.
Palmitoyl-Glu(1)-OH
· Chemical Safety Sheets
Laboratory
Chemical Safety Summary (LCSS) Datasheet
Molecular
Formula
C172H265N43051
The
importance in providing the GLP-1R (EX 4 Liraglutide) to patients with
substance abuse is the perform a case study that provides a taxonomy of
chemical safety data sheets, and treatment diagnosis. Although after reviewing
the chemical compound affects, we declare the treatment for the glycemic index
was the first set of medication trial, to reduce the manifestations of
diabetes, and cravings. Once we controlled the cravings, and diabetes with the
GLP-1R Chemical Depository and Effect Data, the treatment diagnosis, was
properly aligned with a substance abuse case, and underlying condition of
diabetes or glycemic disorders. The glucose disorder causes the cravings and
creates a self-medicating ritual for controlling "body" signals or
receptors. This all explain during the RCT, the chemical compounding, and the
Medications Usage declaration or disclaimer [2] (Figure 2).
Some
methods we use for GLP-1R (EX 4 Liraglutide, was to take a Blood Sample, and we
continued with the Toxicology Tests, and further assigned the participants to a
Addiction Medicine specialists, and substance abuse center. (PubMed, Chem Sci}
After collecting pathology reports over time, we decided to perform a RCT for
OUD participants, the participants were provided with a full report and all had
a underlying condition of glucose disorder, and hepatic disorders. We provided
the organic form of GLP-1R (EX-4 Liraglutide) over a course of 14 days, the
cravings were reduced significantly and remarkably the Toxicology and Pathology
Reports from Quest Laboratory Blood Bank provided us a Statistical Reports of
the reduction of opioids, heroin, cocaine, alcohol, no fentanyl, and marijuana
(THC) [1].
In providing a brief outlook on the GLP-1R, we tracked outcomes by Blood Tests, we adhered to chemical compounding standards (essential medication safety). We controlled the group through a set of Addiction Medicine, and Substance Abuse Compliance Forms. And we set our standards for further study into Chemicals and reactions of substance abuse with medications. Our overview overlooked one issues, which was the issue of blood tests, and type of substance that was used in abusive methods. Our research and our case study summarized that the classification of GLP-1R was properly assigned for treating underlying conditions. Any drug with high levels of H+ or C+ were documented for our next series and Laboratory Biopharmaceuticals Studies. The research covers the GLP-R1 (EX Liraglutide), Chemical Compound information, the diagnosis and prognosis, the Applied Metrics to substance abuse, and Randomized Trials for Opiod Use and Abuse. The research continues on a more in-depth study for Randomized Trials and Substance Abuse by Addiction Medicine Professionals [3-5] (Figure 3).
Figure
3: Participants are randomly assigned to different
treatment groups, iconically the groups are similar at the start of the study.
{EPA, 2011) {Toxic Pharmacol).
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