Impeded Interaction between Schwann Cells and Axons in the Absence of Laminin {alpha}4

doi:10.1523/JNEUROSCI.5225-04.2005

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The Journal of Neuroscience, April 6, 2005, 25(14):3692-3700; doi:10.1523/JNEUROSCI.5225-04.2005

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Cellular/Molecular
Impeded Interaction between Schwann Cells and Axons in the Absence of Laminin ${alpha}$ 4
Wilhelm Wallquist,¹ Stefan Plantman,¹ Sebastian Thams,¹ Jill Thyboll,² Jarkko Kortesmaa,² Jan Lännergren,³ Anna Domogatskaya,² Sven Ove Ögren,¹ Mårten Risling,¹^,4 Henrik Hammarberg,¹^,5 Karl Tryggvason,² and Staffan Cullheim¹
Departments of ¹Neuroscience, ²Medical Biochemistry and Biophysics, and ³Physiology and Pharmacology, Karolinska Institute, 171 77 Stockholm, Sweden, ⁴Department of Defense Medicine, Swedish Defense Research Agency, 171 77 Stockholm, Sweden, and ⁵Department of Hand Surgery, Stockholm Söder Hospital, 118 87 Stockholm, Sweden

The Schwann cell basal lamina (BL) is required for normal myelination.Loss or mutations of BL constituents, such as laminin-2 ( ${alpha}$ 2 ${beta}$ 1 ${gamma}$ 1),lead to severe neuropathic diseases affecting peripheral nerves.The function of the second known laminin present in Schwanncell BL, laminin-8 ( ${alpha}$ 4 ${beta}$ 1 ${gamma}$ 1), is so far unknown. Here we show thatabsence of the laminin ${alpha}$ 4 chain, which distinguishes laminin-8from laminin-2, leads to a disturbance in radial sorting, impairedmyelination, and signs of ataxia and proprioceptive disturbances,whereas the axonal regenerative capacity is not influenced.In vitro studies show poor axon growth of spinal motoneuronson laminin-8, whereas it is extensive on laminin-2. Schwanncells, however, extend longer processes on laminin-8 than onlaminin-2, and, in contrast to the interaction with laminin-2,solely use the integrin receptor ${alpha}$ 6 ${beta}$ 1 in their interaction withlaminin-8. Thus, laminin-2 and laminin-8 have different criticalfunctions in peripheral nerves, mediated by different integrinreceptors.

Key words: myelin; extracellular matrix; Schwann cells; electron microscopy; neuropathy; regeneration

Received July 22, 2004; revised February 21, 2005; accepted February 22, 2005.

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