Distinct iron homeostasis in C57BL/6 and Balb/c mouse strains

Saha, Piu; Xiao, Xia; Li, Yaqi; Golonka, Rachel M.; Abokor, Ahmed A.; Yeoh, Beng San

doi:10.14814/phy2.14441

Cited by 11 publications

(4 citation statements)

References 56 publications

(68 reference statements)

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“…To avoid strain-specific results and limit the potential bias in the assessment of the immune responses, we used distinct HA strains on a C57Bl/6-129 background (colony at CHOP) or BALB/c background (colony at Indiana University). The HA phenotype is similar between these strains but immune responses to pathogens, proteins, and gene therapy is known to differ (58)(59)(60)(61)(62)(63). Further, we used two distinct murine (m) BAFF mAbs: 1) clone 10F4 which is a hamster IgG1 mAb with a half-life of ~2 weeks 64) and 2clone Sandy-2 which is a mouse IgG1 mAb with a half-life of ~10 days (65).…”

Section: Inhibitor Prevention and Eradication Studies In Ha Mouse Modelsmentioning

confidence: 99%

B cell–activating factor modulates the factor VIII immune response in hemophilia A

Doshi¹,

Rana²,

Castaman³

et al. 2021

Journal of Clinical Investigation

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Inhibitors to factor VIII (FVIII) remain the most challenging complication of FVIII protein replacement therapy in hemophilia A (HA). Understanding the mechanisms that guide FVIII-specific B cell development could help identify therapeutic targets. The B cell activating factor (BAFF) cytokine family is a key regulator of B cell differentiation in normal homeostasis and immune disorders. Thus, we used patient samples and mouse models to investigate the potential role of BAFF in modulating FVIII inhibitors. BAFF levels were elevated in pediatric and adult HA inhibitor patients and decreased to levels similar to non-inhibitor controls after successful immune tolerance induction (ITI). Moreover, elevations in BAFF levels were seen in patients who failed to achieve FVIII tolerance with anti-CD20 mediated B-cell depletion. In naïve HA mice, prophylactic anti-BAFF therapy prior to FVIII immunization prevented inhibitors and this tolerance was maintained despite FVIII exposure after immune reconstitution. In preimmunized HA mice, combination therapy with anti-CD20 and anti-BAFF antibodies dramatically reduced FVIII inhibitors via inhibition of FVIII-specific plasma cells. Our data suggest that BAFF may regulate the generation and maintenance of FVIII inhibitors and/or anti-FVIII B cells. Finally, anti-CD20/anti-BAFF combination therapy may be clinically useful for ITI.

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Section: Inhibitor Prevention and Eradication Studies In Ha Mouse Modelsmentioning

confidence: 99%

B cell–activating factor modulates the factor VIII immune response in hemophilia A

Doshi¹,

Rana²,

Castaman³

et al. 2021

Journal of Clinical Investigation

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“…However, this alone was insufficient to induce bone loss under normal conditions in C57BL/6J, implying that the bone could adapt to prevent cell damage caused by iron overload, as the iron content in bone/bone marrow tissues remains unchanged. Moreover, previous reports have indicated that C57BL/6J mice exhibit unique iron characteristics primarily associated with differences in iron absorption capacity on duodenal epithelial cells and iron regulation at the tissue and cellular levels through the expression of hepatic transferrin receptors and ferritin, suggesting that this strain may have a lower capacity for iron uptake and storage in the liver compared to other inbred strains like Balb/c mice 33 . Furthermore, previous reports have indicated that iron accumulation and its effect can vary among different mouse strains, showing that strain differences strongly influence hepatic iron accumulation resulting from an iron-supplemented diet 34 .…”

Section: Discussionmentioning

confidence: 94%

Comparison of the effects of high dietary iron levels on bone microarchitecture responses in the mouse strains 129/Sv and C57BL/6J

Ledesma-Colunga,

Passin,

Vujic Spasic

et al. 2024

Sci Rep

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Iron is an essential nutrient for all living organisms. Both iron deficiency and excess can be harmful. Bone, a highly metabolic active organ, is particularly sensitive to fluctuations in iron levels. In this study, we investigated the effects of dietary iron overload on bone homeostasis with a specific focus on two frequently utilized mouse strains: 129/Sv and C57BL/6J. Our findings revealed that after 6 weeks on an iron-rich diet, 129/Sv mice exhibited a decrease in trabecular and cortical bone density in both vertebral and femoral bones, which was linked to reduced bone turnover. In contrast, there was no evidence of bone changes associated with iron overload in age-matched C57BL/6J mice. Interestingly, 129/Sv mice exposed to an iron-rich diet during their prenatal development were protected from iron-induced bone loss, suggesting the presence of potential adaptive mechanisms. Overall, our study underscores the critical role of genetic background in modulating the effects of iron overload on bone health. This should be considered when studying effects of iron on bone.

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“… 30 In this study, mice on a C57BL/6 background were used, whereas Zhang et al characterized the effect of HJV overexpression in mice on a 129/SvEvTac background. Mice with a different genetic background show differences in iron homeostasis 31 , and it is suggested that the contradictory results are a result of the different genetic mouse backgrounds used in both studies.…”

Section: Discussionmentioning

confidence: 99%

Hemojuvelin-mediated hepcidin induction requires both bone morphogenetic protein type I receptors ALK2 and ALK3

Dogan,

Urzica,

Hornung

et al. 2024

Blood Advances

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Hemojuvelin (HJV) is a GPI-anchored protein of the repulsive guidance molecule (RGM) family acting as a bone morphogenetic protein (BMP) co-receptor to induce the hepatic iron regulatory protein hepcidin. Hepcidin causes ubiquitination and degradation of the sole known iron exporter ferroportin thereby limiting iron availability. The detailed signaling mechanism of HJV in vivo has yet to be investigated. In the current manuscript, we used an established model of adeno-associated virus (AAV) mediated liver-specific overexpression of HJV in murine models of hepatocyte-specific deficiency of the BMP type I receptors Alk2 or Alk3. In control mice, HJV overexpression increased hepatic Hamp mRNA levels, soluble HJV (sHJV), splenic iron content (SIC), as well as pSMAD1/5/8 levels. In contrast, in Alk2fl/fl;Alb-Cre and Alk3fl/fl;Alb-Cre mice, which present with moderate and severe iron overload, respectively, the administration of AAV-HJV induced HJV and sHJV. However, it did not rescue the iron overload phenotypes of those mice. Serum iron levels were induced in Alk2fl/fl;Alb-Cre mice following HJV overexpression. In PBS-injected Alk3fl/fl;Alb-Cre mice serum iron levels and the expression of duodenal ferroportin remained high, whereas Hamp mRNA levels were decreased to 1-5% of the levels detected in controls. This was reduced even further by AAV-HJV overexpression. SIC remained low in mice with hepatocyte-specific Alk2 or Alk3 deficiency, reflecting disturbed iron homeostasis with high serum iron levels and transferrin saturation and an inability to induce hepcidin by HJV overexpression. The data indicate that ALK2 and ALK3 are both required in vivo for the HJV-mediated induction of hepcidin.

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Distinct iron homeostasis in C57BL/6 and Balb/c mouse strains

Cited by 11 publications

References 56 publications

B cell–activating factor modulates the factor VIII immune response in hemophilia A

B cell–activating factor modulates the factor VIII immune response in hemophilia A

Comparison of the effects of high dietary iron levels on bone microarchitecture responses in the mouse strains 129/Sv and C57BL/6J

Hemojuvelin-mediated hepcidin induction requires both bone morphogenetic protein type I receptors ALK2 and ALK3

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