Autocrine IGF-II-Associated Cancers: From a Rare Paraneoplastic Event to a Hallmark in Malignancy

Pierluigi Scalia; Ignazio R Marino; Salvatore Asero; Giuseppe Pandini; Adda Grimberg; Wafik S El-Deiry; Stephen J Williams

doi:10.3390/biomedicines12010040

Autocrine IGF-II-Associated Cancers: From a Rare Paraneoplastic Event to a Hallmark in Malignancy

Biomedicines. 2023 Dec 22;12(1):40. doi: 10.3390/biomedicines12010040.

Authors

Pierluigi Scalia¹, Ignazio R Marino², Salvatore Asero^{1

3}, Giuseppe Pandini¹, Adda Grimberg⁴, Wafik S El-Deiry⁵, Stephen J Williams^{1

6}

Affiliations

¹ The ISOPROG-Somatolink EPFP Research Network, Philadelphia, PA 19102, USA; 93100 Caltanissetta, Italy.
² Department of Surgery, Sidney Kimmel Medical College, Thomas Jefferson University, Philadelphia, PA 19107, USA.
³ ARNAS Garibaldi, UOC Chirurgia Oncologica, Nesima, 95122 Catania, Italy.
⁴ Perelman School of Medicine, University of Pennsylvania, Children's Hospital of Philadelphia, Philadelphia, PA 19104, USA.
⁵ Legorreta Cancer Center, Brown University, Providence, RI 02903, USA.
⁶ Department of Biology, College of Science and Technology, Temple University, Philadelphia, PA 19122, USA.

Abstract

The paraneoplastic syndrome referred in the literature as non-islet-cell tumor hypoglycemia (NICTH) and extra-pancreatic tumor hypoglycemia (EPTH) was first reported almost a century ago, and the role of cancer-secreted IGF-II in causing this blood glucose-lowering condition has been widely established. The landscape emerging in the last few decades, based on molecular and cellular findings, supports a broader role for IGF-II in cancer biology beyond its involvement in the paraneoplastic syndrome. In particular, a few key findings are constantly observed during tumorigenesis, (a) a relative and absolute increase in fetal insulin receptor isoform (IR^A) content, with (b) an increase in IGF-II high-molecular weight cancer-variants (big-IGF-II), and (c) a stage-progressive increase in the IGF-II autocrine signal in the cancer cell, mostly during the transition from benign to malignant growth. An increasing and still under-exploited combinatorial pattern of the IGF-II signal in cancer is shaping up in the literature with respect to its transducing receptorial system and effector intracellular network. Interestingly, while surgical and clinical reports have traditionally restricted IGF-II secretion to a small number of solid malignancies displaying paraneoplastic hypoglycemia, a retrospective literature analysis, along with publicly available expression data from patient-derived cancer cell lines conveyed in the present perspective, clearly suggests that IGF-II expression in cancer is a much more common event, especially in overt malignancy. These findings strengthen the view that (1) IGF-II expression/secretion in solid tumor-derived cancer cell lines and tissues is a broader and more common event compared to the reported IGF-II association to paraneoplastic hypoglycemia, and (2) IGF-II associates to the commonly observed autocrine loops in cancer cells while IGF-I cancer-promoting effects may be linked to its paracrine effects in the tumor microenvironment. Based on these evidence-centered considerations, making the autocrine IGF-II loop a hallmark for malignant cancer growth, we here propose the functional name of IGF-II secreting tumors (IGF-IIsT) to overcome the view that IGF-II secretion and pro-tumorigenic actions affect only a clinical sub-group of rare tumors with associated hypoglycemic symptoms. The proposed scenario provides an updated logical frame towards biologically sound therapeutic strategies and personalized therapeutic interventions for currently unaccounted IGF-II-producing cancers.

Keywords: EPTH; HRA/B; IGF-I-IGF-II (protein); IGF-IR; IGF1-IGF2 (gene); IGF2ST; IGF2oma; IRA; NICTH; NSILA; SpI2-6/IGF-IIR.

Grants and funding

This research received no external funding.