Flexible Players within the Sheaths: The Intrinsically Disordered Proteins of Myelin in Health and Disease

Raasakka, Arne; Kursula, Petri

doi:10.20944/preprints202001.0376.v1

Cited by 7 publications

(12 citation statements)

References 236 publications

(380 reference statements)

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“…The Ig-like domain is structurally very similar to the Ig-like domain in MPZL1, although they share only ~46% sequence identity [ 56 ]. P0ct differs drastically from the Ig-like domain, as it has a compositional bias typical for intrinsically disordered proteins (IDPs) [ 57 ] and is highly positively charged, much like MBP [ 12 , 17 ]. Systematic biophysical characterizations using simplified lipid compositions have been performed on P0ct, which revealed that P0ct alone is an IDP in solution but folds upon irreversible association with negatively charged detergent micelles and lipid vesicles [ 58 , 59 , 60 , 61 ].…”

Section: The Molecular Structure Of P0mentioning

confidence: 99%

“…Experimental evidence suggests that P0ct differs from MBP in one noteworthy aspect during membrane association: when MBP binds to a single membrane, a partially folded intermediate state is formed, which can further adhere to a second membrane given that MBP reaches a critical concentration [ 12 , 63 ]. On the other hand, P0ct as a free polypeptide completely embeds into model membranes ( Figure 3 a) [ 44 ]; however, more studies regarding the binding mode are needed.…”

Section: P0 Is the Executive Pns Membrane Stackermentioning

confidence: 99%

“…When MBP performs its membrane stacking function, local translation of free MBP allows spontaneous interaction with membranes, and the formation of compact myelin [ 63 ]. On the other hand, when MBP remains soluble, it may have other functions [ 12 , 17 ]. The solubility of MBP distinguishes it from the expression pattern and trafficking of P0; P0ct is likely to always remain membrane-embedded and have less spatial freedom.…”

Section: P0 Is the Executive Pns Membrane Stackermentioning

confidence: 99%

“…These in turn arise from the neural crest during early post-natal development along with other glial cells [ 10 ]—a proliferation pathway that is not present in the CNS. Oligodendrocytic myelination in the CNS is arranged differently to that in the PNS [ 11 ], although the mature myelin sheaths in both the CNS and PNS morphologically resemble each other [ 12 ].…”

Section: Introductionmentioning

confidence: 99%

“…CNS and PNS myelin are highly enriched in a mere handful of proteins, which is an unusual feature in most biological systems. Many of these proteins are multifunctional [ 15 , 16 , 17 , 18 , 19 , 20 , 21 ], contain large stretches of intrinsic disorder [ 12 ], tolerate highly hydrophobic conditions [ 22 ], and have extended lifetimes [ 23 ]. While there is some overlap between the CNS and PNS myelin proteomes [ 13 , 14 ], proteins that are specific either to the CNS or the PNS are present especially in compact myelin, which forms the insulative bulk of the myelin sheath.…”

Section: Introductionmentioning

confidence: 99%

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How Does Protein Zero Assemble Compact Myelin?

Raasakka

Kursula

2020

Cells

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Myelin protein zero (P0), a type I transmembrane protein, is the most abundant protein in peripheral nervous system (PNS) myelin—the lipid-rich, periodic structure of membrane pairs that concentrically encloses long axonal segments. Schwann cells, the myelinating glia of the PNS, express P0 throughout their development until the formation of mature myelin. In the intramyelinic compartment, the immunoglobulin-like domain of P0 bridges apposing membranes via homophilic adhesion, forming, as revealed by electron microscopy, the electron-dense, double “intraperiod line” that is split by a narrow, electron-lucent space corresponding to the extracellular space between membrane pairs. The C-terminal tail of P0 adheres apposing membranes together in the narrow cytoplasmic compartment of compact myelin, much like myelin basic protein (MBP). In mouse models, the absence of P0, unlike that of MBP or P2, severely disturbs myelination. Therefore, P0 is the executive molecule of PNS myelin maturation. How and when P0 is trafficked and modified to enable myelin compaction, and how mutations that give rise to incurable peripheral neuropathies alter the function of P0, are currently open questions. The potential mechanisms of P0 function in myelination are discussed, providing a foundation for the understanding of mature myelin development and how it derails in peripheral neuropathies.

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Section: The Molecular Structure Of P0mentioning

confidence: 99%

Section: P0 Is the Executive Pns Membrane Stackermentioning

confidence: 99%

Section: P0 Is the Executive Pns Membrane Stackermentioning

confidence: 99%

Section: Introductionmentioning

confidence: 99%

Section: Introductionmentioning

confidence: 99%

See 3 more Smart Citations

How Does Protein Zero Assemble Compact Myelin?

Raasakka

Kursula

2020

Cells

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How Does Protein Zero Assemble Compact Myelin?

Raasakka

Kursula

2020

Preprint

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Myelin protein zero (P0), a type I transmembrane protein, is the most abundant protein in peripheral nervous system (PNS) myelin – the lipid-rich, periodic structure that concentrically encloses long axonal segments. Schwann cells, the myelinating glia of the PNS, express P0 throughout their development until the formation of mature myelin. In the intramyelinic compartment, the immunoglobulin-like domain of P0 bridges apposing membranes together via homophilic adhesion, forming a dense, macroscopic ultrastructure known as the intraperiod line. The C-terminal tail of P0 adheres apposing membranes together in the narrow cytoplasmic compartment of compact myelin, much like myelin basic protein (MBP). In mouse models, the absence of P0, unlike that of MBP or P2, severely disturbs the formation of myelin. Therefore, P0 is the executive molecule of PNS myelin maturation. How and when is P0 trafficked and modified to enable myelin compaction, and how disease mutations that give rise to incurable peripheral neuropathies alter the function of P0, are currently open questions. The potential mechanisms of P0 function in myelination are discussed, providing a foundation for the understanding of mature myelin development and how it derails in peripheral neuropathies.

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Emerging cellular themes in leukodystrophies

Nowacki

Fields

2022

Front. Cell Dev. Biol.

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Leukodystrophies are a broad spectrum of neurological disorders that are characterized primarily by deficiencies in myelin formation. Clinical manifestations of leukodystrophies usually appear during childhood and common symptoms include lack of motor coordination, difficulty with or loss of ambulation, issues with vision and/or hearing, cognitive decline, regression in speech skills, and even seizures. Many cases of leukodystrophy can be attributed to genetic mutations, but they have diverse inheritance patterns (e.g., autosomal recessive, autosomal dominant, or X-linked) and some arise from de novo mutations. In this review, we provide an updated overview of 35 types of leukodystrophies and focus on cellular mechanisms that may underlie these disorders. We find common themes in specialized functions in oligodendrocytes, which are specialized producers of membranes and myelin lipids. These mechanisms include myelin protein defects, lipid processing and peroxisome dysfunction, transcriptional and translational dysregulation, disruptions in cytoskeletal organization, and cell junction defects. In addition, non-cell-autonomous factors in astrocytes and microglia, such as autoimmune reactivity, and intercellular communication, may also play a role in leukodystrophy onset. We hope that highlighting these themes in cellular dysfunction in leukodystrophies may yield conceptual insights on future therapeutic approaches.

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Flexible Players within the Sheaths: The Intrinsically Disordered Proteins of Myelin in Health and Disease

Cited by 7 publications

References 236 publications

How Does Protein Zero Assemble Compact Myelin?

How Does Protein Zero Assemble Compact Myelin?

How Does Protein Zero Assemble Compact Myelin?

Emerging cellular themes in leukodystrophies

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