European Journal of Histochemistry (Mar 2009)

Different prelamin A forms accumulate in human fibroblasts: a study in experimental models and progeria

  • G Lattanzi,
  • NM Maraldi,
  • C Vigouroux,
  • G Novelli,
  • M Caron,
  • M Auclair,
  • C Le Dour,
  • MR D’Apice,
  • D Camozzi,
  • C Capanni,
  • E Schena,
  • M Magnani,
  • V Fiori,
  • S Dominici

DOI
https://doi.org/10.4081/ejh.2009.43
Journal volume & issue
Vol. 53, no. 1
pp. 43 – 52

Abstract

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Lamin A is a component of the nuclear lamina mutated in a group of human inherited disorders known as laminopathies. Among laminopathies, progeroid syndromes and lipodystrophies feature accumulation of prelamin A, the precursor protein which, in normal cells, undergoes a multi-step processing to yield mature lamin A. It is of utmost importance to characterize the prelamin A form accumulated in each laminopathy, since existing evidence shows that drugs acting on protein processing can improve some pathological aspects.We report that two antibodies raised against differently modified prelamin A peptides show a clear specificity to full-length prelamin A or carboxymethylated farnesylated prelamin A, respectively. Using these antibodies, we demonstrated that inhibition of the prelamin A endoprotease ZMPSTE24 mostly elicits accumulation of full-length prelamin A in its farnesylated form, while loss of the prelamin A cleavage site causes accumulation of carboxymethylated prelamin A in progeria cells. These results suggest a major role of ZMPSTE24 in the first prelamin A cleavage step.