Saudi Journal of Medicine and Medical Sciences

REVIEW ARTICLE
Year
: 2022  |  Volume : 10  |  Issue : 3  |  Page : 183--191

Tyrosine kinase targeting: A potential therapeutic strategy for diabetes


Mohammad Althubiti 
 Department of Biochemistry, Faculty of Medicine, Umm Al-Qura University, Makkah, Saudi Arabia

Correspondence Address:
Mohammad Althubiti
Department of Biochemistry, Faculty of Medicine, Umm Al-Qura University, Prince Sultan Road 5096, Makkah
Saudi Arabia

Abstract

Tyrosine kinase inhibitors (TKIs) have been studied extensively in cancer research, ultimately resulting in the approval of many drugs for cancer therapy. Recent evidence from reported clinical cases and experimental studies have suggested that some of these drugs have a potential role in diabetes treatment. These TKIs include imatinib, sunitinib, dasatinib, erlotinib, nilotinib, neratinib, and ibrutinib. As a result of promising findings, imatinib has been used in a phase II clinical trial. In this review, studies that used TKIs in the treatment of both types of diabetes are critically discussed. In addition, the different molecular mechanisms of action of these drugs in diabetes models are also highlighted to understand their antidiabetic mode of action.



How to cite this article:
Althubiti M. Tyrosine kinase targeting: A potential therapeutic strategy for diabetes.Saudi J Med Med Sci 2022;10:183-191


How to cite this URL:
Althubiti M. Tyrosine kinase targeting: A potential therapeutic strategy for diabetes. Saudi J Med Med Sci [serial online] 2022 [cited 2022 Oct 3 ];10:183-191
Available from: https://www.sjmms.net/text.asp?2022/10/3/183/355698


Full Text



 Introduction



Protein tyrosine kinases (PTKs) promote the addition of phosphate groups to target proteins, thus modulating their activity. Downregulation of PTK activity by various mechanistic alterations has implications for cellular proliferative activity, especially during malignant transformation.[1] Activation of PTKs results in increased cancer cell growth, induces anti-apoptotic actions, and promotes angiogenesis.[2] Specific tyrosine kinase inhibitors (TKIs) have been developed as a result of the deep understanding of the enzyme network activity. Several cases of improvement in patients with type 1 (T1D) and type 2 diabetes (T2D) during TKI treatment have been documented. These observations have also been supported by in vivo studies, which have uncovered the mechanism of action of these agents, and have resulted in the entry of imatinib into a clinical trial for the treatment of early onset T1D.[3]

Diabetes mellitus is a metabolic disease resulting from chronic elevation of blood glucose levels due to impairment in insulin secretion and activity. T1D is initiated as a result of an autoimmune system that destroys pancreatic β cells in combination with immune cell infiltration and cytokine and reactive oxygen species (ROS) secretion, ultimately causing β-cell apoptosis.[4] In this type of diabetes, the disorder usually progresses for years before chronic hyperglycemia is noticed.[4]

T2D is a complicated disorder characterized by a decrease in the sensitivity of the target tissue towards insulin action. This results in chronic hyperglycemia and hyperinsulinemia, and ultimately pancreatic β-cell exhaustion and dysfunction. Resistance to insulin action is strongly correlated with obesity, especially in the visceral region, and chronic inflammation from the adipose tissue of the abdomen.[5] In adipose tissue, macrophages produce cytokines, such as interleukin-6 and tumor necrosis factor-alpha, which augment inflammation and adipocyte impairment, resulting in the release of free fatty acids and inhibition of adiponectin production.

As a result of this scenario, kinases, such as nuclear factor kappa-light-chain-enhancer of activated B cells (NF-κB) and c-Jun N-terminal kinase (JNK) are upregulated. These enzymes induce phosphorylation of the insulin receptor and insulin receptor substrate (IRS) on serine residues, thereby inhibiting their phosphorylation on tyrosine residues, which results in the inhibition of insulin signaling and maintenance of high glucose levels in the bloodstream.[6] However, β cells respond to insulin resistance by increasing insulin production; subsequently, they become exhausted and impaired. There is a multifactorial etiology behind the inability of β cells to overcome insulin resistance. Free fatty acid release, proinflammatory mediators, oxidative stress, and chronic hyperglycemia all contribute to the gradual damage of β cell activity.[6]

Insulin replacement therapy is the only therapy available for patients with T1D; no other safe interventions may be used for stopping immune destruction or regeneration of β-cells.[4] In addition, the current anti-diabetic drugs for T2D do not prevent or ameliorate β-cell dysfunction.[7] Thus, there is a demand for new intervention models that solve the etiology of T1D and T2D. In this review, the anti-diabetic effects of TKIs from available studies on humans and animals in both types of diabetes are critically discussed. In addition, the possible mode of action of TKIs on diabetes will be analyzed considering studies conducted in humans, in vivo animal models, and in vitro cell lines. The antidiabetic effects of TKIs have been reported from clinical observations and from studies in animals for both T1D and T2D, as shown in [Table 1].{Table 1}

To extract relevant articles for this review, PubMed searches were carried out between March 2020 until the beginning of 2021 using the following keywords: <Diabetes, tyrosine kinase inhibitor>; <diabetes, treatment, tyrosine kinase inhibitor>; <Type 1 diabetes, tyrosine kinase inhibitor>; <Type 2 diabetes, tyrosine kinase inhibitor>; <Insulin, tyrosine kinase inhibitor>; <Hyperglycemia, tyrosine kinase inhibitor>; < Insulin resistance, tyrosine kinase inhibitor>; <Insulin secretion, tyrosine kinase inhibitor>.

 Type 1 Diabetes



Clinical evidence

Many lines of evidence reveal that TKIs have antidiabetic properties in patients with T1D. In a patient with chronic myeloid leukemia (CML) who had T1D and was taking imatinib, the quantity of regular insulin intake decreased and a significant improvement in blood glucose concentrations was observed.[8] In addition, administration of sunitinib to a patient with pancreatic tumor who had T1D resulted in a reduction of his diabetic condition, such that he stopped insulin treatment for 12 weeks after starting sunitinib therapy[9] and improvement in glucose and hemoglobin A1c (HbA1c) levels was observed. In addition, diabetes improvement has been observed in patients with T1D diagnosed with renal cell carcinoma (RCC).[26] The patient started treatment with sunitinib for 8 months, after which insulin therapy was reduced.

Blood glucose levels and HbA1c were normal without antidiabetic drugs for approximately 7 months [Table 1]. A more selective TKI, ibrutinib, which targets Bruton's tyrosine kinase, shows an antidiabetic effect in two reported cases with chronic lymphocytic leukemia and T1D. Doses of insulin injection are lowered after administration of ibrutinib as a result of severe hypoglycemia and decreased levels of circulating insulin antibodies.[47]

Evidence from experimental studies

There is evidence from animal and in vitro studies supporting clinical observations of the antidiabetic effects of TKIs in T1D treatment.

Imatinib has shown antidiabetic action in nonobese diabetic (NOD) mice that are genetically similar to T1D, and also in diabetic mice induced by streptozotocin (STZ). The onset of diabetes was prevented in prediabetic NOD mice, partially prevented in mice that received STZ after administration of imatinib, and showed some protection of human pancreatic β cells through reduction of nitric oxide (NO).[9] These findings were confirmed by another study that found imatinib administration to a group of prediabetic NOD mice provided protection from diabetes onset.[10] However, a few mice progressed to diabetes after treatment termination, while diabetes reappeared in two-thirds of diabetic NOD animals after imatinib withdrawal. Nonetheless, imatinib withdrawal after extended administration led to prolonged diabetes reduction. In addition, imatinib has also been shown to induce insulin synthesis from NOD animals and protects human pancreatic β cells [Figure 1].[11],[12]{Figure 1}

A previous study has tested the potential anti-apoptotic action of imatinib and two other TKIs (GNF-2 and GNF-5) in STZ-induced diabetic animals;[13] all three TKIs have anti-apoptotic activity for β cells in vitro. Moreover, blood glucose levels were maintained within the normal range in STZ-induced mice after GNF-2 administration, whereas the effect was milder in mice that received GNF-5 [Table 1]. In addition, pancreatic tissue of STZ-induced diabetes animals treated with imatinib mesylate has low levels of oxidative stress and high antioxidant capacity.[15] The study also showed lower levels of tissue injury and higher insulin content in the treated animals.[15]

Another TKI drug, sunitinib, has been shown to ameliorate T1D in NOD animals in the first week of administration, and with diabetes reoccurring in only six mice, 9 weeks after drug injection.[10] In addition, T1D mice induced by alloxan have shown a decrease in blood glucose levels due to a single dose of sunitinib.[27] A more recent study that examined the mechanism by which sunitinib increases insulin secretion found that the drug directly stimulates glucose insulin secretion from pancreatic β-cells.[28]

Another study used a micelle polymer to encapsulate sunitinib, thereby increasing its release efficiency.[29] NOD T1D mice that received this formulation systematically showed a decrease in blood glucose levels. In addition, the diabetic animals responded rapidly to the drug, as determined by a glucose tolerance test, and the survival and activity of islet cells also increased in parallel with a reduction in immune cell infiltration.[29]

Erlotinib has also shown antidiabetic effects in mice treated with STZ; importantly, the treated mice showed less cardiomyopathy and less fibrotic tissue in the heart and decrease in the genes responsible for fibrosis and hypertrophy in cardiomyocytes.[38] However, it is not clear whether the later observations were from the antidiabetic effects of the drug.

These in vivo data confirmed that TKIs not only reverse T1D, but also prevent the onset of the disease. The possible proposed mechanism of their antidiabetic effect is possibly through protecting β cells from apoptosis and stimulation of insulin synthesis and secretion. Recently, imatinib reversed hyperglycemia in T1D NOD mice through B-lymphocyte modulation. Imatinib increases the antioxidant capacity of B lymphocytes and enhances ROS status in NOD mouse islet cells.[14] In fact, further work should focus on the mechanism of action of these drugs to identify any possible side effects.

As a result of the promising effect of TKIs on T1D, imatinib has been used in clinical trials. A phase II trial is underway for the treatment of early onset T1D. However, the trail has not proceeded to phase III, as no data on the pediatric population are available.[3]

 Type 2 Diabetes



Clinical evidence

There is strong evidence of the antidiabetic role of TKIs in T2D. For example, patients with different cancer types who had T2D and were treated with imatinib or other TKIs showed a reduction in blood glucose levels, followed by a decrease or cessation of antidiabetic treatment.[17] Imatinib showed a long-acting antidiabetic action after the treatment session, while cessation of other TKIs led to diabetes reoccurrence. Similar findings were observed in seven patients with T2D who had CML and received imatinib; they showed diabetes amelioration and controlled blood glucose levels that resulted in a decrease in the dose of antidiabetic drugs.[18] Moreover, imatinib treatment in a patient with CML and T2D resulted in normalized blood glucose concentration and HbA1c levels,[19] while another patient with the same tumor type and T2D discontinued insulin replacement therapy, and blood glucose levels normalized.[20] A recent study included 106 patients with CML or stromal cell cancer and T2D who were treated with imatinib and had a significant decrease in blood glucose and HbA1c levels at 1 and 6 months when using the drug.[21] These clinical data support the potential antidiabetic effect of imatinib.

Sunitinib has been shown to reverse T2D. There are documented cases of patients with RCC and T2D, whose blood glucose levels normalized after 2 weeks of sunitinib therapy, leading to the withdrawal of prescribed antidiabetic medicine.[30] Ten patients with RCC and T2D who were treated with sunitinib demonstrated a significant decrease in blood glucose levels, followed by decreasing or even cessation of antidiabetic therapy.[31] In contrast, after 2 weeks of treatment cessation, blood glucose levels rose. The same results were observed in 19 patients with RCC with T2D;[32] 1-month after treatment with sunitinib, blood glucose levels were reduced and then elevated after drug withdrawal.

Regarding another TKI, dasatinib, a case study showed that it normalized blood glucose levels in a patient with CML and T2D, and resulted in insulin therapy cessation and increased C-peptide in the blood.[35] Another study also found that dasatinib administration in a patient with CML and T2D ameliorated diabetes.[36] In addition, a study reported that a patient with T2D, who had been treated with metformin, was later diagnosed with CML. Subsequently, dasatinib was introduced as a therapy for the cancer, and later, glucose levels improved and HbA1c levels became more controlled.[37]

Finally, erlotinib is another TKI showing an effect on T2D by exhibiting an antidiabetic effect in two patients with T2D and non-small cell lung cancer.[39],[49] In these patients, erlotinib caused a clear reduction in blood glucose levels, leading to the discontinuation of regular diabetes treatment.[39]

However, there are reported cases of the opposite effects of TKIs on diabetes. For example, use of nilotinib has shown the opposite effect in many reported studies. Nilotinib treatment in patients with CML showed a reduction in insulin secretion, leading to the introduction of insulin therapy until termination of the nilotinib therapy.[42] In addition, a recent retrospective analysis of the incidence of T2D in patients who had CML and were treated with nilotinib showed a higher incidence rate of diabetes. However, the study assessed the risk of developing T2D, including different age groups rather than the antidiabetic potential of the drug, and the patients treated with nilotinib and erlotinib were compared.[43] A prospective study on patients with CML who were treated with nilotinib for 12 months showed a significant increase in blood glucose levels.[44]

Evidence from experimental studies

There is evidence of the effect of TKIs in in vivo and in vitro models of T2D. Db/db mice, a genetic model of T2D, treated with imatinib normalize blood glucose levels by increasing β cell size and improving insulin action on the target tissue.[43] Moreover, addition of imatinib has been found to abolish the induction of insulin resistance and high glucose levels in rats.[23] The antidiabetic effect of imatinib has been reported in another study; it decreases random blood glucose in parallel with insulin resistance and inflammatory biomarkers in ob/ob mice.[24] A subsequent study showed that imatinib exerts positive effects on the metabolism of glucose and fat, resulting in improved insulin signaling.[22] Spontaneously diabetic Torii rats, a non-obese model of type 2 diabetes, treated with sunitinib show a remarkable reduction in blood glucose levels.[33]

In addition, erlotinib has been shown to have antidiabetic effects in db/db mice. Treated mice have shown lowered blood glucose, improved glucose tolerance and insulin action, and increased adiponectin levels compared to controls.[40] In addition, the treated animals presented fewer diabetic complications compared with the untreated mice. Interestingly, treatment of high-fat diet mice with nilotinib increases insulin sensitivity and decreases fat mass,[45] which contradicts the clinical data of the adverse effects of nilotinib on glucose impairment. One possible explanation is that clinical observations[42],[44] have focused on insulin secretion rather than insulin action. Another probable reason is that nilotinib may have off-target effects that may include dual effects of insulin.

Recently, neratinib has demonstrated antidiabetic activity. Neratinib improves β-cell proliferation and activity in vitro.[46] Neratinib decreased blood glucose levels and improved β cell activity and size after STZ injection as well as in obese mouse models. Gefitinib, which targets receptor-interacting serine/threonine-protein kinase-2, also decreases glucose levels in a glucose tolerance test in an insulin-resistant animal model by increasing insulin action.[50] Another recent example of a TKI with antidiabetic activity is ibrutinib. In vitro, ibrutinib increases glucose transportation inside cells and decreases the production of inflammatory cytokines from treated cells.[48]

Previous studies in experimental models of T2D [Table 1] have emphasized the clinical evidence of the potential role of TKIs as antidiabetic agents by increasing β cell mass and activity, decreasing inflammatory responses, and enhancing insulin sensitivity, which subsequently improved blood glucose levels.

 Mechanism Of Action Of Tkis as Antidiabetic Drugs



The potential mechanisms by which TKIs exert their effects as antidiabetic agents may vary and depend primarily on which TK is targeted [Figure 1]. Alternatively, for some TKIs, such as imatinib, the mechanism of its antidiabetic activity is not fully understood.

Abelson non-receptor tyrosine kinase (c-Abl) pathway

c-Abl is a non-receptor tyrosine kinase that activates β cell apoptosis when it becomes active.[9] It contributes to the control of cellular cytoskeleton functions, such as cell shape, cell cycle upregulation, and movement.[51] However, when cells are under stress from oxidation, for example, c-Abl activity is induced, resulting in cell cycle regression and apoptosis,[52] by upregulating JNK[53] and downregulating NF-κB activity.[9] Therefore, imatinib, when targeting c-Abl, may prevent β cell apoptosis in diabetic conditions. In addition, a study shows that imatinib and two other c-Abl molecule inhibitors (GNF-2 and GNF-5) protect β cells from death due to STZ.[13] Targeting c-Abl reduces JNK, caspase-3, and protein kinase C γ levels, which are known to promote β cell apoptosis. Furthermore, another study showed that c-Abl induces β cell apoptosis in NOD mice by binding to inositol-requiring transmembrane kinase/endoribonuclease 1α (IRE1α), which damages the endoplasmic reticulum to induce apoptosis. Imatinib reduces c-Abl and IRE1α binding diminishes IRE1α action, which subsequently protects and reverses β cell T1D.[16]

C-Abl modulates insulin synthesis and secretion, demonstrating the inhibitory effect of c-Abl on insulin secretion from β cells.[54] The negative role of c-Abl in insulin secretion is through downregulation of NK2 homeobox 2 and glucose transporter 2, which normally induce insulin production in glucose-positive conditions.[11] In parallel, targeting c-Abl increased insulin secretion by β cells.

Another finding proposes that imatinib targeting c-Abl activity increases in vitro human β cell growth and survival.[12] The study also shows that imatinib activates phosphatidylinositol-4,5-bisphosphate 3-kinase (PI3K), protein kinase B, and β-catenin signaling, which is essential for β cell activity.[12] In fact, β-catenin is a central modulator of the Wnt and protein kinase B pathways, and upregulation of β-catenin increases survival and growth of different cells, including β cells.[55] C-Abl phosphorylates SH2-domain-containing inositol phosphatase 2 (SHIP2) and inhibits PI3K and β-catenin activity. This subsequently decreases the capacity of β cells for proliferation and activity.[12] In this event, c-Abl inhibition by imatinib reverses its negative role in β cell survival and proliferation through activation of SHIP2 and PI3K.

Adiponectin, a positive modulator of insulin sensitivity, increases after imatinib treatment.[56] In vitro studies have shown that the drug accelerates adipocyte differentiation and elevates adiponectin production. Platelet-derived growth factor receptor (PDGFR), a downstream target of c-Abl, has been shown to be an important effector.[57] Lastly, antidiabetic properties of c-Abl downregulation may be linked to activation of low-density lipoprotein receptor-related protein 1, which transduces extracellular signal-regulated kinase activation.[56]

PDGFR pathway

PDGFR is another PTK that may be targeted for therapeutic purposes.[57] It not only has proliferative and growing effects under physiological conditions, but is also involved in the progression of many chronic disorders, such as atherosclerosis and pulmonary and renal fibrosis.[58]

PDGFR activity is increased in diabetes through high blood glucose levels and low adiponectin and peroxisome proliferator-activated receptor (PPAR)-λ. These cause upregulation of the PDGFR pathway, leading to a decrease in insulin sensitivity in the target tissue.[59],[60] Hence, it is possible that targeting PDGFR may increase insulin action and ameliorate diabetes. As stated previously, using imatinib, which targets a pathway that involves PDGFR, increases adiponectin through a mechanism that depends on PDGFR inhibition.[61] PPAR-λ is blocked after imatinib administration, which increases insulin sensitivity.[22]

Tyrosine-protein kinase KIT (c-Kit) pathway

c-Kit is another kinase targeted by imatinib and is less affected by sunitinib and dasatinib.[57] It is involved in the growth and differentiation of pancreatic cells, among other cells.[62] c-Kit upregulation in β cells increases their proliferation and activity and prevents the development of diabetes in animal models.[63] These results suggest that c-Kit performs a physiological function in β cells; thus, its targeting by TKIs may have adverse effects on diabetes. This concept has been confirmed by studies that reveal that c-Kit inhibition does not selectively normalize blood glucose in diabetic mice,[29] and amelioration in vivo by TKIs works independently of c-Kit.[64]

Vascular endothelial growth factor receptor pathway

This enzyme is targeted by sunitinib among other TKIs; targeting vascular endothelial growth factor receptor (VEGFR) has shown antidiabetic properties. VEGFR2 signaling controls angiogenesis, while VEGFR1 signaling performs opposite events.[65] VEGFR ligands play a role in inflammation and white blood cell recruitment by increasing the expression of cytokines and chemokines.[66],[67] Blocking VEGFR2 signaling through TKIs normalized the blood glucose levels and ameliorated diabetes. In addition, it was shown that targeting VEGFR2 decreased T cell recruitment into β cells of the pancreas as well as inflammation. These findings have been documented in other studies, where VEGFR2 inhibition decreased insulitis.[33]

Epidermal growth factor receptor pathway

Epidermal growth factor receptor (EGFR) downregulation has been proposed to have antidiabetic properties. This finding is reported in db/db mice, where targeting EGFR improves blood glucose levels, and increases glucose tolerance and insulin action.[40] Moreover, EGFR decreases proinflammatory cytokines and immune cell recruitment in renal tissue, leading to less diabetic complications compared with controls.[40] EGFR-signal transducer and activator of transcription 3 (STAT3) signaling may play a role in diabetes. A study reporting in vivo and in vitro models of diabetes showed an interaction between EGFR and STAT3 in cardiomyopathy resulting from diabetes complications. Blocking EGFR inhibits STAT3 phosphorylation and decreases cardiomyopathy in diabetic mice, in parallel with genes that play a role in fibrosis and hypertrophy in cardiomyocytes.[38]

 Off-Tarket Effects Of TKIs



Although TKI drugs have been designed to target and inhibit specific modulators of pathways, off-target effects are commonly seen in such therapies. There are some documented examples of TKI off-target effects in diabetes. A recent study showed the effects of neratinib, the drug that has been approved for metastatic human epidermal growth factor receptor 2-positive breast cancer,[68] and showed antidiabetic activity in T1D and T2D animal models. However, neratinib exerts this effect through different molecular mechanisms.[46] The use of a knockout mouse model showed that the drug worked mainly through blocking the activity of the transcription factor MTS1 in β cells. Therefore, some of the TKIs that have been discussed may show an antidiabetic effect through off-targeting effects. In the future, more precise methodology using knockout mouse models is required to illustrate the exact mechanism by which TKIs exert antidiabetic properties.

 Conclusions



TKIs have been widely used as therapeutic regimens for different cancers. Accumulating evidence has proposed the antidiabetic actions of these TKIs in both types of diabetes. Clinical and experimental data showed that some of them have potent effects on T1D, while others affect T2D. In contrast, some TKIs, such as erlotinib, interestingly, induced or augmented diabetes in studies. Therefore, understanding the molecular mechanism of TKIs in diabetes is very important before proceeding with experimental data from clinical trials.

Peer review

This article was peer-reviewed by four independent and anonymous reviewers.

Financial support and sponsorship

Nil.

Conflicts of interest

There are no conflicts of interest.

References

1Roskoski R Jr. Properties of FDA-approved small molecule protein kinase inhibitors. Pharmacol Res 2019;144:19-50.
2Pottier C, Fresnais M, Gilon M, Jérusalem G, Longuespée R, Sounni NE. Tyrosine kinase inhibitors in cancer: Breakthrough and challenges of targeted therapy. Cancers (Basel) 2020;12:E731.
3Imatinib Treatment in Recent Onset Type 1 Diabetes Mellitus. NIH; 2020. Available from: https://www.clinicaltrials.gov/ct2/show/study/NCT01781975. [Last cited on 2020 Dec 01].
4Craig ME, Kim KW, Isaacs SR, Penno MA, Hamilton-Williams EE, Couper JJ, et al. Early-life factors contributing to type 1 diabetes. Diabetologia 2019;62:1823-34.
5Czech MP. Insulin action and resistance in obesity and type 2 diabetes. Nat Med 2017;23:804-14.
6Shimobayashi M, Albert V, Woelnerhanssen B, Frei IC, Weissenberger D, Meyer-Gerspach AC, et al. Insulin resistance causes inflammation in adipose tissue. J Clin Invest 2018;128:1538-50.
7Park YJ, Woo M. Pancreatic β cells: Gatekeepers of type 2 diabetes. J Cell Biol 2019;218:1094-5.
8Salaroli A, Loglisci G, Serrao A, Alimena G, Breccia M. Fasting glucose level reduction induced by imatinib in chronic myeloproliferative disease with TEL-PDGFRβ rearrangement and type 1 diabetes. Ann Hematol 2012;91:1823-4.
9Hägerkvist R, Sandler S, Mokhtari D, Welsh N. Amelioration of diabetes by imatinib mesylate (Gleevec): Role of beta-cell NF-kappaB activation and anti-apoptotic preconditioning. FASEB J 2007;21:618-28.
10Louvet C, Szot GL, Lang J, Lee MR, Martinier N, Bollag G, et al. Tyrosine kinase inhibitors reverse type 1 diabetes in nonobese diabetic mice. Proc Natl Acad Sci U S A 2008;105:18895-900.
11Xia CQ, Zhang P, Li S, Yuan L, Xia T, Xie C, et al. C-Abl inhibitor imatinib enhances insulin production by β cells: c-Abl negatively regulates insulin production via interfering with the expression of NKx2.2 and GLUT-2. PLoS One 2014;9:e97694.
12Mokhtari D, Al-Amin A, Turpaev K, Li T, Idevall-Hagren O, Li J, et al. Imatinib mesilate-induced phosphatidylinositol 3-kinase signalling and improved survival in insulin-producing cells: Role of Src homology 2-containing inositol 5'-phosphatase interaction with c-Abl. Diabetologia 2013;56:1327-38.
13Karunakaran U, Park SJ, Jun do Y, Sim T, Park KG, Kim MO, et al. Non-receptor tyrosine kinase inhibitors enhances β-cell survival by suppressing the PKCδ signal transduction pathway in streptozotocin-induced β-cell apoptosis. Cell Signal 2015;27:1066-74.
14Wilson CS, Spaeth JM, Karp J, Stocks BT, Hoopes EM, Stein RW, et al. B lymphocytes protect islet β cells in diabetes prone NOD mice treated with imatinib. JCI Insight 2019;5:e125317.
15Samaha MM, Said E, Salem HA. Modulatory role of imatinib mesylate on pancreatic β-cells' secretory functions in an STZ rat model of diabetes mellitus. Chem Biol Interact 2020;328:109197.
16Morita S, Villalta SA, Feldman HC, Register AC, Rosenthal W, Hoffmann-Petersen IT, et al. Targeting ABL-IRE1α signaling spares ER-stressed pancreatic β cells to reverse autoimmune diabetes. Cell Metab 2017;25:883-97.e8.
17Agostino NM, Chinchilli VM, Lynch CJ, Koszyk-Szewczyk A, Gingrich R, Sivik J, et al. Effect of the tyrosine kinase inhibitors (sunitinib, sorafenib, dasatinib, and imatinib) on blood glucose levels in diabetic and nondiabetic patients in general clinical practice. J Oncol Pharm Pract 2011;17:197-202.
18Breccia M, Muscaritoli M, Aversa Z, Mandelli F, Alimena G. Imatinib mesylate may improve fasting blood glucose in diabetic Ph+chronic myelogenous leukemia patients responsive to treatment. J Clin Oncol 2004;22:4653-5.
19Breccia M, Muscaritoli M, Alimena G. Reduction of glycosylated hemoglobin with stable insulin levels in a diabetic patient with chronic myeloid leukemia responsive to imatinib. Haematologica 2005;90 Suppl: ECR21.
20Veneri D, Franchini M, Bonora E. Imatinib and regression of type 2 diabetes. N Engl J Med 2005;352:1049-50.
21Gómez-Sámano MÁ, Baquerizo-Burgos JE, Coronel MF, Wong-Campoverde BD, Villanueva-Martinez F, Molina-Botello D, et al. Effect of imatinib on plasma glucose concentration in subjects with chronic myeloid leukemia and gastrointestinal stromal tumor. BMC Endocr Disord 2018;18:77.
22Choi SS, Kim ES, Jung JE, Marciano DP, Jo A, Koo JY, et al. PPARγ Antagonist Gleevec Improves Insulin Sensitivity and Promotes the Browning of White Adipose Tissue. Diabetes 2016;65:829-39.
23Hägerkvist R, Jansson L, Welsh N. Imatinib mesylate improves insulin sensitivity and glucose disposal rates in rats fed a high-fat diet. Clin Sci (Lond) 2008;114:65-71.
24Lim YM, Lim H, Hur KY, Quan W, Lee HY, Cheon H, et al. Systemic autophagy insufficiency compromises adaptation to metabolic stress and facilitates progression from obesity to diabetes. Nat Commun 2014;5:4934.
25Huda MS, Amiel SA, Ross P, Aylwin SJ. Tyrosine kinase inhibitor sunitinib allows insulin independence in long-standing type 1 diabetes. Diabetes Care 2014;37:e87-8.
26Templeton A, Brändle M, Cerny T, Gillessen S. Remission of diabetes while on sunitinib treatment for renal cell carcinoma. Ann Oncol 2008;19:824-5.
27Szałek E, Karbownik A, Sobańska K, Grabowski T, Połom W, Lewandowska M, et al. The pharmacokinetics and hypoglycaemic effect of sunitinib in the diabetic rabbits. Pharmacol Rep 2014;66:892-6.
28Lutz SZ, Ullrich A, Häring HU, Ullrich S, Gerst F. Sunitinib specifically augments glucose-induced insulin secretion. Cell Signal 2017;36:91-7.
29Peng Y, Wen D, Lin F, Mahato RI. Co-delivery of siAlox15 and sunitinib for reversing the new-onset of type 1 diabetes in non-obese diabetic mice. J Control Release 2018;292:1-12.
30Demirci A, Bal O, Durnali A, Ekinci AŞ, Eşbah O, Alkiş N, et al. Sunitinib-induced severe hypoglycemia in a diabetic patient. J Oncol Pharm Pract 2014;20:469-72.
31Oh JJ, Hong SK, Joo YM, Lee BK, Min SH, Lee S, et al. Impact of sunitinib treatment on blood glucose levels in patients with metastatic renal cell carcinoma. Jpn J Clin Oncol 2012;42:314-7.
32Billemont B, Medioni J, Taillade L, Helley D, Meric JB, Rixe O, et al. Blood glucose levels in patients with metastatic renal cell carcinoma treated with sunitinib. Br J Cancer 2008;99:1380-2.
33Mukai E, Ohta T, Kawamura H, Lee EY, Morita A, Sasase T, et al. Enhanced vascular endothelial growth factor signaling in islets contributes to β cell injury and consequential diabetes in spontaneously diabetic Torii rats. Diabetes Res Clin Pract 2014;106:303-11.
34Yu L, Liu J, Huang X, Jiang Q. Adverse effects of dasatinib on glucose-lipid metabolism in patients with chronic myeloid leukaemia in the chronic phase. Sci Rep 2019;9:17601.
35Ono K, Suzushima H, Watanabe Y, Kikukawa Y, Shimomura T, Furukawa N, et al. Rapid amelioration of hyperglycemia facilitated by dasatinib in a chronic myeloid leukemia patient with type 2 diabetes mellitus. Intern Med 2012;51:2763-6.
36Breccia M, Muscaritoli M, Cannella L, Stefanizzi C, Frustaci A, Alimena G. Fasting glucose improvement under dasatinib treatment in an accelerated phase chronic myeloid leukemia patient unresponsive to imatinib and nilotinib. Leuk Res 2008;32:1626-8.
37Iizuka K, Niwa H, Kato T, Takeda J. Dasatinib improves insulin sensitivity and affects lipid metabolism in a patient with chronic myeloid leukaemia. BMJ Case Rep 2016;2016:bcr2015214284.
38Luo W, Huang L, Wang J, Zhuang F, Xu Z, Yin H, et al. Inhibition of EGFR-STAT3 attenuates cardiomyopathy in streptozotocin-induced type 1 diabetes. J Endocrinol 2019;242:199-210.
39Costa DB, Huberman MS. Improvement of type 2 diabetes in a lung cancer patient treated with Erlotinib. Diabetes Care 2006;29:1711.
40Li Z, Li Y, Overstreet JM, Chung S, Niu A, Fan X, et al. Inhibition of epidermal growth factor receptor activation is associated with improved diabetic nephropathy and insulin resistance in type 2 diabetes. Diabetes 2018;67:1847-57.
41Samaha MM, Said E, Salem HA. Nilotinib enhances β-islets integrity and secretory functions in a rat model of STZ-induced diabetes mellitus. Eur J Pharmacol 2019;860:172569.
42Ito Y, Miyamoto T, Chong Y, Maki T, Akashi K, Kamimura T. Nilotinib exacerbates diabetes mellitus by decreasing secretion of endogenous insulin. Int J Hematol 2013;97:135-8.
43Franklin M, Burns L, Perez S, Yerragolam D, Makenbaeva D. Incidence of type 2 diabetes mellitus and hyperlipidemia in patients prescribed dasatinib or nilotinib as first- or second-line therapy for chronic myelogenous leukemia in the US. Curr Med Res Opin 2018;34:353-60.
44Racil Z, Koritakova E, Sacha T, Klamova H, Belohlavkova P, Faber E, et al. Insulin resistance is an underlying mechanism of impaired glucose metabolism during nilotinib therapy. Am J Hematol 2018;93:E342-5.
45Wu R, Sun JG, Wang JQ, Li B, Liu Q, Ning G, et al. c-Abl inhibition mitigates diet-induced obesity through improving insulin sensitivity of subcutaneous fat in mice. Diabetologia 2017;60:900-10.
46Ardestani A, Li S, Annamalai K, Lupse B, Geravandi S, Dobrowolski A, et al. Neratinib protects pancreatic beta cells in diabetes. Nat Commun 2019;10:5015.
47Skrabs C, Pickl WF, Perkmann T, Jäger U, Gessl A. Rapid decline in insulin antibodies and glutamic acid decarboxylase autoantibodies with ibrutinib therapy of chronic lymphocytic leukaemia. J Clin Pharm Ther 2018;43:145-9.
48Althubiti M, Almaimani R, Eid SY, Elzubaier M, Refaat B, Idris S, et al. BTK targeting suppresses inflammatory genes and ameliorates insulin resistance. Eur Cytokine Netw 2020;31:168-79.
49Brooks MB. Erlotinib and gefitinib, epidermal growth factor receptor kinase inhibitors, may treat non-cancer-related tumor necrosis factor-α mediated inflammatory diseases. Oncologist 2013;18:e3-5.
50Duggan BM, Cavallari JF, Foley KP, Barra NG, Schertzer JD. RIPK2 dictates insulin responses to tyrosine kinase inhibitors in obese male mice. Endocrinology 2020;161:bqaa086.
51Sirvent A, Benistant C, Roche S. Cytoplasmic signalling by the c-Abl tyrosine kinase in normal and cancer cells. Biol Cell 2008;100:617-31.
52Houstis N, Rosen ED, Lander ES. Reactive oxygen species have a causal role in multiple forms of insulin resistance. Nature 2006;440:944-8.
53Hägerkvist R, Makeeva N, Elliman S, Welsh N. Imatinib mesylate (Gleevec) protects against streptozotocin-induced diabetes and islet cell death in vitro. Cell Biol Int 2006;30:1013-7.
54Halperin F, Lopez X, Manning R, Kahn CR, Kulkarni RN, Goldfine AB. Insulin augmentation of glucose-stimulated insulin secretion is impaired in insulin-resistant humans. Diabetes 2012;61:301-9.
55Bernal-Mizrachi E, Kulkarni RN, Scott DK, Mauvais-Jarvis F, Stewart AF, Garcia-Ocaña A. Human β-cell proliferation and intracellular signaling part 2: still driving in the dark without a road map. Diabetes 2014;63:819-31.
56Fred RG, Boddeti SK, Lundberg M, Welsh N. Imatinib mesylate stimulates low-density lipoprotein receptor-related protein 1-mediated ERK phosphorylation in insulin-producing cells. Clin Sci (Lond) 2015;128:17-28.
57Rask-Andersen M, Zhang J, Fabbro D, Schiöth HB. Advances in kinase targeting: Current clinical use and clinical trials. Trends Pharmacol Sci 2014;35:604-20.
58Heldin CH, Westermark B. Mechanism of action and in vivo role of platelet-derived growth factor. Physiol Rev 1999;79:1283-316.
59Campbell M, Allen WE, Silversides JA, Trimble ER. Glucose-induced phosphatidylinositol 3-kinase and mitogen-activated protein kinase-dependent upregulation of the platelet-derived growth factor-beta receptor potentiates vascular smooth muscle cell chemotaxis. Diabetes 2003;52:519-26.
60Raines SM, Richards OC, Schneider LR, Schueler KL, Rabaglia ME, Oler AT, et al. Loss of PDGF-B activity increases hepatic vascular permeability and enhances insulin sensitivity. Am J Physiol Endocrinol Metab 2011;301:E517-26.
61Fitter S, Vandyke K, Gronthos S, Zannettino AC. Suppression of PDGF-induced PI3 kinase activity by imatinib promotes adipogenesis and adiponectin secretion. J Mol Endocrinol 2012;48:229-40.
62Krishnamurthy M, Ayazi F, Li J, Lyttle AW, Woods M, Wu Y, et al. c-Kit in early onset of diabetes: A morphological and functional analysis of pancreatic β-Cells in c-KitW-v mutant mice. Endocrinology 2007;148:5520-30.
63Feng ZC, Li J, Turco BA, Riopel M, Yee SP, Wang R. Critical role of c-Kit in beta cell function: increased insulin secretion and protection against diabetes in a mouse model. Diabetologia 2012;55:2214-25.
64Lau J, Zhou Q, Sutton SE, Herman AE, Schmedt C, Glynne R. Inhibition of c-Kit is not required for reversal of hyperglycemia by imatinib in NOD mice. PLoS One 2014;9:e84900.
65Lacal PM, Graziani G. Therapeutic implication of vascular endothelial growth factor receptor-1 (VEGFR-1) targeting in cancer cells and tumor microenvironment by competitive and non-competitive inhibitors. Pharmacol Res 2018;136:97-107.
66Scaldaferri F, Vetrano S, Sans M, Arena V, Straface G, Stigliano E, et al. VEGF-A links angiogenesis and inflammation in inflammatory bowel disease pathogenesis. Gastroenterology 2009;136:585- 95.e5.
67Boulday G, Haskova Z, Reinders ME, Pal S, Briscoe DM. Vascular endothelial growth factor-induced signaling pathways in endothelial cells that mediate overexpression of the chemokine IFN-gamma-inducible protein of 10 kDa in vitro and in vivo. J Immunol 2006;176:3098-107.
68FDA. FDA approves neratinib for metastatic HER2-positive breast cancer. In: Administration USFD, editor. United States: FDA; 2020.