Protein structure may aid in treating Alzheimerâs disease
Vanderbilt University Medical Center Research News May 03, 2017
The protein gamma–secretase appeared to be a promising target for drugs to treat AlzheimerÂs disease. It Âcuts the amyloid precursor protein to release amyloid–beta  a protein fragment that clumps together and forms neuron–killing plaques.
ÂAmyloid–beta is thought to Âseed AlzheimerÂs disease, so lowering its production has been a goal to prevent, or possibly treat, the disease, said Charles Sanders, PhD, Aileen M. Lange and Annie Mary Lyle Professor of Cardiovascular Research at Vanderbilt.
However, although inhibitors of gamma–secretase successfully reduce the production of amyloid–beta, participants in previous clinical trials experienced side effects including skin cancers and reduced cognitive abilities.
The problem, Sanders said, is that in addition to cutting the amyloid precursor protein (APP), gamma–secretase also cuts other proteins. And one of these proteins, called Notch, needs to be cut to initiate a signaling pathway that is important to multiple cellular functions.
ÂIf you inhibit gamma–secretase, you reduce amyloid–beta production, which is good, but you also inhibit Notch cleavage, leading to cancer and other disorders, said Sanders, who is also professor of Biochemistry and Medicine.
Sanders and his team had previously solved the molecular structure of the APP region that is cut by gamma–secretase to generate amyloid–beta.
Now, in research led by Catherine Deatherage, PhD, the investigators have solved the molecular structure of the corresponding region of Notch, to look for differences that might guide the development of selective inhibitors.
They reported in the journal Science Advances that Âthe way the Notch region is shaped and the way it interacts with the membrane is distinctly different from APP, Sanders said. They also discovered that, in contrast to APP, the Notch region does not bind cholesterol.
The differences Âprovide hope to an old idea that it might be possible to develop compounds that selectively interact with either of these proteins and/or with gamma–secretase in a way that inhibits the APP pathway but leaves the Notch pathway alone, Sanders said.
The cholesterol–binding region in APP, but not Notch, is of particular interest, he noted. Drugs called gamma–secretase modulators appear to bind to the cholesterol–binding region of APP, but they have not been clinically successful inhibitors of gamma–secretase action.
ÂOur structure gives an extra bit of information that may allow drug development to go a step further than it could before, Sanders said.
The clinical failures of drugs that attempt to block amyloid–beta production have made the idea that amyloid–beta initiates AlzheimerÂs disease controversial, Sanders said.
ÂI think we havenÂt tried the right things yet, and IÂm still hopeful that this is a pathway that can be targeted, he said.
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ÂAmyloid–beta is thought to Âseed AlzheimerÂs disease, so lowering its production has been a goal to prevent, or possibly treat, the disease, said Charles Sanders, PhD, Aileen M. Lange and Annie Mary Lyle Professor of Cardiovascular Research at Vanderbilt.
However, although inhibitors of gamma–secretase successfully reduce the production of amyloid–beta, participants in previous clinical trials experienced side effects including skin cancers and reduced cognitive abilities.
The problem, Sanders said, is that in addition to cutting the amyloid precursor protein (APP), gamma–secretase also cuts other proteins. And one of these proteins, called Notch, needs to be cut to initiate a signaling pathway that is important to multiple cellular functions.
ÂIf you inhibit gamma–secretase, you reduce amyloid–beta production, which is good, but you also inhibit Notch cleavage, leading to cancer and other disorders, said Sanders, who is also professor of Biochemistry and Medicine.
Sanders and his team had previously solved the molecular structure of the APP region that is cut by gamma–secretase to generate amyloid–beta.
Now, in research led by Catherine Deatherage, PhD, the investigators have solved the molecular structure of the corresponding region of Notch, to look for differences that might guide the development of selective inhibitors.
They reported in the journal Science Advances that Âthe way the Notch region is shaped and the way it interacts with the membrane is distinctly different from APP, Sanders said. They also discovered that, in contrast to APP, the Notch region does not bind cholesterol.
The differences Âprovide hope to an old idea that it might be possible to develop compounds that selectively interact with either of these proteins and/or with gamma–secretase in a way that inhibits the APP pathway but leaves the Notch pathway alone, Sanders said.
The cholesterol–binding region in APP, but not Notch, is of particular interest, he noted. Drugs called gamma–secretase modulators appear to bind to the cholesterol–binding region of APP, but they have not been clinically successful inhibitors of gamma–secretase action.
ÂOur structure gives an extra bit of information that may allow drug development to go a step further than it could before, Sanders said.
The clinical failures of drugs that attempt to block amyloid–beta production have made the idea that amyloid–beta initiates AlzheimerÂs disease controversial, Sanders said.
ÂI think we havenÂt tried the right things yet, and IÂm still hopeful that this is a pathway that can be targeted, he said.
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