# Basement membrane self-assembly and structure

> **NIH NIH R01** · RBHS-ROBERT WOOD JOHNSON MEDICAL SCHOOL · 2022 · $357,750

## Abstract

Abstract: Basement membranes (BMs) are extracellular matrices (ECMs) containing laminins, collagen-IV,
nidogens and proteoglycans as structural elements. They provide mechanical support for cells and act as 
signaling platforms. Laminins mediate BM assembly by adhering to cells, by establishing cytoskeletal links
through receptors, by polymerizing, and by recruiting the other BM components. These cell-adherent ECMs
are essential for tissue growth, differentiation, and maintenance, attributes that depend upon BM molecular
architecture and receptor-binding. Diseases of BMs can result from structural changes that adversely affect
muscle, peripheral nerve, kidney and other organs. The long-term goal of the grant is to elucidate mechanisms
of BM assembly and architecture-dependent functions. This goal is critical for understanding BM disease 
pathogenesis and for developing therapies for BM defects. We now seek to determine how BMs can be modified
to regain lost function in neuromuscular and renal diseases, explore the molecular basis of laminin 
polymerization, and elucidate architectural properties of BMs that determine functions.
 Aim I. Mutations ablating the polymerization laminin α2 subunit result in ambulatory muscular dystrophy
(LAMA2-MD) with peripheral nerve amyelination. We succeeded in ameliorating the muscle component of a
mouse (dy2J) model of polymerization-deficient dystrophy by transgenic muscle expression of a laminin-
binding linker-protein called αLNNd. This leads us to evaluate this protein for repair of the peripheral nerve
component of the disease. The aim holds potential for development of a therapy by viral somatic gene delivery.
 Aim II. Proteins conferring polymerization (αLNNd) and dystroglycan (αDG) receptor-binding (miniagrin,
mag) to laminins have been used to ameliorate the severe muscle disease resulting from absent laminin-α2
(dy3K mice). The benefit results from modification of compensatory α4 laminin that otherwise neither 
polymerizes nor binds to αDG. Normal assembly and functions of α4-laminins will be explored, focusing particularly on
peripheral nerve myelination. We plan to complete an analysis of transgene muscle expression in the dy3K
mouse, and evaluate αLNNd and mag in Lmα2-null peripheral nerve to determine if this ameliorates the 
paresis. The aim is expected to elucidate laminin contributions needed for myelination and contribute to 
development of a therapy to treat muscle and nerve in LAMA2-MD arising from total loss of the α2 subunit.
 Aim III. BM-binding proteins can be engineered to alter BM assembly and functions by increasing receptor
binding, inducing polymerization, and altering inter-component binding and spacing. We propose to use these
unique reagents to determine if the human laminin mutations that cause dystrophies and renal Pierson 
syndrome are due to failures of laminin polymerization, to map the polymerization residues on laminin LN domain
surfaces accompanied by a structural analysis ...

## Key facts

- **NIH application ID:** 10440388
- **Project number:** 5R01DK036425-38
- **Recipient organization:** RBHS-ROBERT WOOD JOHNSON MEDICAL SCHOOL
- **Principal Investigator:** PETER Dana YURCHENCO
- **Activity code:** R01 (R01, R21, SBIR, etc.)
- **Funding institute:** NIH
- **Fiscal year:** 2022
- **Award amount:** $357,750
- **Award type:** 5
- **Project period:** 1986-01-01 → 2024-06-30

## Primary source

NIH RePORTER: https://reporter.nih.gov/project-details/10440388

## Citation

> US National Institutes of Health, RePORTER application 10440388, Basement membrane self-assembly and structure (5R01DK036425-38). Retrieved via AI Analytics 2026-05-23 from https://api.ai-analytics.org/grant/nih/10440388. Licensed CC0.

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