Increased synthesis of heparin affin regulatory peptide in the perforant path lesioned mouse hippocampal formation

F. R. Poulsen, C. Lagord, J. Courty, E. B. Pedersen, D. Barritault, B. Finsen

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20 Citations (Scopus)


Heparin affin regulatory peptide (HARP), also known as pleiotrophin or heparin-binding growth-associated molecule, is a developmentally regulated extracellular matrix protein that induces cell proliferation and promotes neurite outgrowth in vitro as well as pre- and postsynaptic developmental differentiation in vivo. Here we have investigated the expression of HARP mRNA and protein in the perforant path lesioned C57B1/6 mouse hippocampal formation from 1 to 35 days after surgery. This type of lesion induces a dense anterograde and terminal axonal degeneration, activation of glial cells, and reactive axonal sprouting within the perforant path zones of the fascia dentata and hippocampus as well as axotomy-induced retrograde neuronal degeneration in the entorhinal cortex. Analysis of sham- and unoperated control mice showed that HARP mRNA is expressed in neurons and white and gray matter glial cells as well as vascular and pial cells throughout the normal, adult brain. Lesioning induced high levels of HARP mRNA in astroglial-like cells in the denervated zones of fascia dentata and hippocampus as soon as day 2 postlesion. This expression reached maximum at day 4, and declined toward normal at day 7-14. Combined HARP in situ hybridization and glial fibrillary acidic protein (GFAP) immunohistochemical staining and double immunofluorescent stainings for GFAP and HARP at day 4 postlesion showed colocalization of HARP mRNA and protein to hypertrophic GFAP-immunopositive astrocytes in the denervated areas. Finally, the axotomized entorhinal layer II neurons, which expressed high levels of HARP mRNA in the normal brain, exhibited a marked decline in hybridization signal after axotomy. The induction of high levels of HARP mRNA and protein in astrocytes in the denervated areas of fascia dentata and hippocampus is of particular interest as astrocytes and astrocyte-derived factors are known to be implicated in axonal growth and regeneration and in rescuing injured neurons.

Original languageEnglish
Pages (from-to)319-330
Number of pages12
JournalExperimental Brain Research
Issue number3
Publication statusPublished - 2000
Externally publishedYes

Bibliographical note

Funding Information:
Acknowledgements We would like to thank technicians Grethe Jensen, Inger Margrethe Rasmussen, Jacob Bang Jensen, Lene Jørgensen, and Dorete Jensen for excellent technical assistance. Albert Meier is thanked for photographic assistance. Profs. Ann Logan and D. Caruelle are thanked for their continuous support. The study was supported by a European BIOMED contract number CT94–1168 and received additional financial support from the Danish MRC, P.A. Messerschmidt and wife's Foundation, and SDU – Odense University, as well as from the French CNRS and Ministère de l'Education Nationale.


  • Astrocytes
  • Degeneration
  • Growth factors
  • HARP
  • Hippocampus
  • Regeneration
  • Sprouting


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