Malard1: A Potential Drug Target for Neurological Disorders (G340895)

Malard1: A Potential Drug Target for Neurological Disorders

Malard1 (also known as DIET1) is a protein that is expressed in the brain and is involved in the development and progression of several neurological disorders, including Alzheimer's disease. The Malard1 protein has been identified as a potential drug target (or biomarker) due to its unique structure and the diseases it is associated with.

The Malard1 protein is composed of 120 amino acid residues and has a calculated molecular weight of 13.9 kDa. It is located in the brain and is expressed in the white matter, which is the tissue that makes up the brain's messaging system. The protein is involved in the formation of the blood-brain barrier, which is a barrier that separates the brain from the surrounding blood vessels and is thought to contribute to the development of several neurological disorders.

One of the unique features of the Malard1 protein is its ability to cross the blood-brain barrier. This is an important function for the protein, as the barrier is designed to prevent the entry of foreign particles into the brain. However, studies have shown that Malard1 is able to cross the barrier and interact with other proteins in the brain, which suggests that it may play a role in the development of certain neurological disorders.

Another potential mechanism by which Malard1 may contribute to the development of neurological disorders is its role in the formation of neurodegenerate structures. The neurodegenerate structures that are formed as a result of the Malard1 protein's activity are thought to contribute to the development of conditions such as Alzheimer's disease. These structures include neurofibrillary tangles and senile plaques, which are thought to be responsible for the progressive neurodegeneration that is observed in Alzheimer's disease.

In addition to its role in the formation of neurodegenerate structures, Malard1 is also involved in the regulation of synaptic plasticity, which is the ability of the brain to change and adapt over time. Studies have shown that the Malard1 protein is involved in the regulation of the neurotransmitter glutamate, which is a critical molecule involved in synaptic plasticity. This suggests that the protein may play a role in the treatment of conditions such as Alzheimer's disease, which are characterized by the loss of synaptic plasticity.

Another potential mechanism by which Malard1 may contribute to the development of neurological disorders is its role in the regulation of inflammation. The brain is home to a network of immune cells that are responsible for protecting the body from infection and inflammation. However, the presence of these immune cells is thought to contribute to the development of certain neurological disorders. Studies have shown that the Malard1 protein is involved in the regulation of the immune response, which suggests that it may play a role in the development of conditions such as multiple sclerosis.

In conclusion, Malard1 is a protein that is expressed in the brain and is involved in the development and progression of several neurological disorders. Its unique structure and ability to cross the blood-brain barrier make it an attractive potential drug target. The protein's involvement in the formation of neurodegenerate structures and the regulation of synaptic plasticity, as well as its role in the regulation of inflammation, make it a promising target for the development of new treatments for neurological disorders. Further research is needed to fully understand the role of Malard1 in the development of neurological disorders and to develop effective treatments.

Protein Name: MAM And LDL Receptor Class A Domain Containing 1

Functions: Enhances production and/or transport of FGF19 and thus has a role in regulation of bile acid synthesis

The "MALRD1 Target / Biomarker Review Report" is a customizable review of hundreds up to thousends of related scientific research literature by AI technology, covering specific information about MALRD1 comprehensively, including but not limited to:
•   general information;
•   protein structure and compound binding;
•   protein biological mechanisms;
•   its importance;
•   the target screening and validation;
•   expression level;
•   disease relevance;
•   drug resistance;
•   related combination drugs;
•   pharmacochemistry experiments;
•   related patent analysis;
•   advantages and risks of development, etc.
The report is helpful for project application, drug molecule design, research progress updates, publication of research papers, patent applications, etc. If you are interested to get a full version of this report, please feel free to contact us at BD@silexon.ai

More Common Targets

MALSU1 | MALT1 | MAMDC2 | MAMDC2-AS1 | MAMDC4 | MAML1 | MAML2 | MAML3 | MAMLD1 | MAMSTR | MAN1A1 | MAN1A2 | MAN1B1 | MAN1B1-DT | MAN1C1 | MAN2A1 | MAN2A2 | MAN2B1 | MAN2B2 | MAN2C1 | MANBA | MANBAL | MANCR | MANEA | MANEA-DT | MANEAL | MANF | MANSC1 | MANSC4 | MAOA | MAOB | MAP10 | MAP1A | MAP1B | MAP1LC3A | MAP1LC3B | MAP1LC3B2 | MAP1LC3BP1 | MAP1LC3C | MAP1S | MAP2 | MAP2K1 | MAP2K1P1 | MAP2K2 | MAP2K3 | MAP2K4 | MAP2K4P1 | MAP2K5 | MAP2K6 | MAP2K7 | MAP3K1 | MAP3K10 | MAP3K11 | MAP3K12 | MAP3K13 | MAP3K14 | MAP3K14-AS1 | MAP3K15 | MAP3K19 | MAP3K2 | MAP3K2-DT | MAP3K20 | MAP3K20-AS1 | MAP3K21 | MAP3K3 | MAP3K4 | MAP3K5 | MAP3K5-AS2 | MAP3K6 | MAP3K7 | MAP3K7CL | MAP3K8 | MAP3K9 | MAP3K9-DT | MAP4 | MAP4K1 | MAP4K1-AS1 | MAP4K2 | MAP4K3 | MAP4K3-DT | MAP4K4 | MAP4K5 | MAP6 | MAP6D1 | MAP7 | MAP7D1 | MAP7D2 | MAP7D3 | MAP9 | MAPK1 | MAPK10 | MAPK10-AS1 | MAPK11 | MAPK12 | MAPK13 | MAPK14 | MAPK15 | MAPK1IP1L | MAPK3 | MAPK4