Injection-site Malignant Fibrous Histiocytomas in a Pegvisomant Carcinogenicity Study in SD Rats

Bartholomew, Phillip M.; Kreeger, John M.; Morton, Daniel G.

doi:10.1177/0192623313517772

Cited by 3 publications

(3 citation statements)

References 28 publications

(32 reference statements)

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“…Administration-site MFH is a well-known finding and has been reported in rodent long-term studies with drugs, nongenotoxic chemicals, plant extracts, and inert materials when administered or implanted sc (Bartholomew, Kreeger, and Morton 2014;Thomas et al 1977). Chronic irritation and inflammation were considered to constitute the key etiologic trigger of administration-site MFH (Thomas et al 1977;Stammberger et al 2002;Bartholomew, Kreeger, and Morton 2014). Interestingly, administration-site MFH was seen in preclinical rodent studies with a number of other marketed drugs (Bartholomew, Kreeger, and Morton 2014).…”

Section: Overview On Repeated Dose Toxicity Studies Evaluated In Thismentioning

confidence: 99%

“…In a 12-month toxicity study in rats with insulin glulisine and 24-month carcinogenicity studies both in rats and mice with insulin glargine, respectively, treatmentrelated malignant fibrous histiocytoma (MFH) was diagnosed in male and, occasionally, in female rats and mice (Greaves and Faccini 1981;Ward et al 1981) of most groups, including the vehicle control group, at the sc administration site on a background of chronic irritation and inflammation (Stammberger et al 2002; European Medicines Evaluation Agency [EMEA], 2005). Administration-site MFH is a well-known finding and has been reported in rodent long-term studies with drugs, nongenotoxic chemicals, plant extracts, and inert materials when administered or implanted sc (Bartholomew, Kreeger, and Morton 2014;Thomas et al 1977). Chronic irritation and inflammation were considered to constitute the key etiologic trigger of administration-site MFH (Thomas et al 1977;Stammberger et al 2002;Bartholomew, Kreeger, and Morton 2014).…”

Section: Overview On Repeated Dose Toxicity Studies Evaluated In This Reviewmentioning

confidence: 99%

“…Chronic irritation and inflammation were considered to constitute the key etiologic trigger of administration-site MFH (Thomas et al 1977; Stammberger et al 2002; Bartholomew, Kreeger, and Morton 2014). Interestingly, administration-site MFH was seen in preclinical rodent studies with a number of other marketed drugs (Bartholomew, Kreeger, and Morton 2014). Even after decades of clinical use of insulin and insulin analogues, no reports of administration-site MFH or other injection-site neoplasia in diabetic patients were identified in the available literature.…”

Section: Target Organs Of Insulins and Insulin Analogues In Preclinical Toxicity Studiesmentioning

confidence: 99%

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Regulatory Forum Opinion Piece

et al. 2016

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The toxicological profile of insulins is exclusively due to exaggerated pharmacology resulting in hypoglycemic findings. Insulin analogues displaying modifications and aimed at improving pharmacokinetics do not induce different toxicity. The main target is the brain displaying neuronal necrosis. Wallerian degeneration of nerves occurs rarely after severe hypoglycemia. These findings are of potential human relevance; nevertheless, these changes are induced in normoglycemic animals whereas diabetic patients suffer from hyperglycemia. Therefore, it is usually not difficult to achieve a therapeutic window for subsequent use in patients. Based upon this and in the absence of classical toxicity, there has been no scientific need for diabetic animal models. A greater challenge is the mitogenicity already inherent with regular insulin. Thus, the focus for preclinical safety evaluation of analogues is to demonstrate that modifications in regular insulin do not result in enhanced mitogenicity. The approaches used to assess the mitogenic potential of insulin analogues have changed over time driven by scientific progression and changes within the regulatory environment. Therefore, in vitro and in vivo evaluation of cell proliferation has become common practice, and to date there has been no evidence that the mitogenic potential of insulin analogues may be increased compared to regular insulin.

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Section: Overview On Repeated Dose Toxicity Studies Evaluated In Thismentioning

confidence: 99%

Section: Overview On Repeated Dose Toxicity Studies Evaluated In This Reviewmentioning

confidence: 99%

Section: Target Organs Of Insulins and Insulin Analogues In Preclinical Toxicity Studiesmentioning

confidence: 99%

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Regulatory Forum Opinion Piece

et al. 2016

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Unwanted disorders and xenogeneic graft‐versus‐host disease in experimental immunodeficient mice: How to evaluate and how to report

Monzavi,

Muhammadnejad,

Mansouri

et al. 2024

Anim Models and Exp Med

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Human‐derived tumor models are essential for preclinical development of new anticancer drug entities. Generating animal models bearing tumors of human origin, such as patient‐derived or cell line–derived xenograft tumors, is dependent on immunodeficient strains. Tumor‐bearing immunodeficient mice are susceptible to developing unwanted disorders primarily irrelevant to the tumor nature; and if get involved with such disorders, reliability of the study results will be undermined, inevitably confounding the research in general. Therefore, a rigorous health surveillance and clinical monitoring system, along with the establishment of a strictly controlled barrier facility to maintain a pathogen‐free state, are mandatory. Even if all pathogen control and biosafety measures are followed, there are various noninfectious disorders capable of causing tissue and multiorgan damage in immunodeficient animals. Therefore, the researchers should be aware of sentinel signs to carefully monitor and impartially report them. This review discusses clinical signs of common unwanted disorders in experimental immunodeficient mice, and how to examine and report them.

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