Neurotensin is an autocrine trophic factor stimulated by androgen withdrawal in human prostate cancer

  1. I Sehgal,
  2. S Powers,
  3. B Huntley,
  4. G Powis,
  5. M Pittelkow, and
  6. N J Maihle
  1. Department of Biochemistry, Mayo Clinic, Rochester, MN 55905.

Abstract

After therapeutic hormone deprivation, prostate cancer cells often develop androgen-insensitive growth through mechanisms thus far undefined. Neuropeptides have been previously implicated as growth factors in some prostate cancers. Here, we demonstrate that androgen-sensitive LNCaP human prostate cancer cells produce and secrete neurotensin following androgen withdrawal. We show that while LNCaP cells express the neurotensin receptor, only androgen-deprived cells exhibit a growth response to exogenous neurotensin. We further demonstrate that androgen-stimulated cells may be refractory to exogenous neurotensin due to androgen induction of a metalloprotease active toward neurotensin. Thus, prostate cancer cells deprived of androgen develop an alternative autocrine growth mechanism involving neurotensin.

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  1. PNAS May 24, 1994 vol. 91 no. 11 4673-4677
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