The gene encoding rat insulinlike growth factor-binding protein 1 is rapidly and highly induced in regenerating liver.

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Mol Cell Biol. 1991 March; 11(3): 1393-1401

The gene encoding rat insulinlike growth factor-binding protein 1 is rapidly and highly induced in regenerating liver.

K L Mohn, A E Melby, D S Tewari, T M Laz and R Taub

Department of Human Genetics, University of Pennsylvania School of Medicine, Philadelphia 19104-6145.

ABSTRACT

The liver is an epithelioid organ that can regenerate followingpartial hepatectomy. Although it is composed mainly of hepatocytes,it has a complex, multicellular architecture, implying thatintercellular communications must exist during regeneration.As in other mitogen-stimulated cells, immediate-early growthresponse genes induced in the absence of prior protein synthesisare likely to play an important regulatory role in the regenerativeprocess. Through differential screening of regenerating livercDNA libraries, we found that one of the most highly expressedimmediate-early genes in liver regeneration encodes the rathomolog of the low-molecular-weight insulinlike growth factor(IGF)-binding protein (IGFBP-1). This protein has been implicatedin enhancing the mitogenic effect of IGF on tissues. IGFBP-1gene induction is transcriptionally mediated and specific toregenerating liver, as the gene is not expressed in mitogen-stimulatedfibroblasts. IGFBP-1 expression has been shown to increase underlow-insulin conditions such as diabetes, and the complex regulationof expression is indicated by our finding that insulin treatmentof H35 rat hepatoma cells, which induces proliferation, alsocauses a rapid decrease in transcription and expression of theIGFBP-1 gene. Of note, IGFBP-1 mRNA is abundant in fetal ratliver, implying that it participates in normal liver growthand development. Although regenerating liver cells continueto produce IGF-I, we did not detect IGF-I receptor mRNA duringthe first 24 h after hepatectomy. However, some IGFBPs may actto enhance the activity of IGF-I independently of IGF-I receptors.Thus, IGF-1 and IGFBPs may interact with hepatocytes or nonparenchymalliver cells, through either IGF-I or novel receptors. In thisway, IGFBP-I and IGF-I could act in a paracrine and/or autocrinefashion in maintaining normal liver architecture during regeneration.

Mol Cell Biol. 1991 March; 11(3): 1393-1401

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