Specific Hemosiderin Deposition in Spleen Induced by a Low Dose of Cisplatin: Altered Iron Metabolism and Its Implication as an Acute Hemosiderin Formation Model

Wang, Yingze; Lv, Juan; Ma, Xiaowei; Wang, Dongliang; Ma, Huili; Chang, Yan‐Zhong; Nie, Guangjun; Jia, Lee; Duan, Xingguang; Liang, Xing‐Jie

doi:10.2174/138920010791636149

Cited by 47 publications

(27 citation statements)

References 41 publications

Supporting

Mentioning

Contrasting

Unclassified

Order By: Relevance

“…The reduction of Hb concentration is due to erythrocyte damage induced by CP. These results are in agreement with those obtained by Wang et al who speculated that the splenic injury and hemosiderin deposition might be mainly due to abnormal erythrocyte damage induced by CP. Moreover, our data are consistent with those of Sachs and Lotem and Mazur et al who reported that CP toxicity, at therapeutic doses, to bone marrow cells was evident and probably CP can trigger apoptosis and affect cell cycle causing anemia and a decrease in TLC.…”

Section: Discussionsupporting

confidence: 93%

Cinnamic Acid and Cinnamaldehyde Ameliorate Cisplatin-Induced Splenotoxicity in Rats

El‐Raouf

El-Sayed

Manie

2015

J Biochem Mol Toxicol

View full text Add to dashboard Cite

Cinnamic acid (CA) and cinnamaldehyde (CD) are major constituents of cinnamon species. They possess various pharmacological properties of which their antioxidant activity is a prime one. This study aims to investigate potential protective effects against cisplatin (CP)-induced splenotoxicity in rats. A single dose of CP (5 mg/kg) injected i.p. caused a significant decrease in hemoglobin content (18%), total leucocytic count (46%), neutrophils (78%), and catalase (CAT) splenic activity (64%) with a marked increase in lymphocytes (26%) and splenic content of malondialdehyde (68%) and TNF-α (69%) as compared with the control group. Contrarily, CA (50 mg/kg, p.o.) or CD (40 mg/kg, p.o.) administration for 7 days before CP ameliorated CP-induced splenotoxicity as indicated by mitigation of the biochemical parameters and histopathological changes. These results revealed the promising protective effects of CA and CD on CP-induced splenotoxicity in rats; an effect that might be attributed to antioxidant and anti-inflammatory activities.

show abstract

Section: Discussionsupporting

confidence: 93%

Cinnamic Acid and Cinnamaldehyde Ameliorate Cisplatin-Induced Splenotoxicity in Rats

El‐Raouf

El-Sayed

Manie

2015

J Biochem Mol Toxicol

View full text Add to dashboard Cite

show abstract

“…Interestingly, brown staining was observed in the spleen from vorinostat or vorinostat and ABT-888 treated mice (panel 'a' in S7 Fig ). It has been noted before that accumulation of hemosiderin in the spleen of cisplatin-treated mice was associated with brown staining in H&E stained preparations [ 34 ]. Indeed Prussian blue staining revealed an increased level of splenic iron in vorinostat or vorinostat and ABT-888 treated mice (panel 'b' in S7 Fig ).…”

Section: Resultsmentioning

confidence: 99%

Overcoming Resistance of Cancer Cells to PARP-1 Inhibitors with Three Different Drug Combinations

Yalon¹,

Tuval-Kochen²,

Castel³

et al. 2016

PLoS ONE

View full text Add to dashboard Cite

Inhibitors of poly[ADP-ribose] polymerase 1 (PARPis) show promise for treatment of cancers which lack capacity for homologous recombination repair (HRR). However, new therapeutic strategies are required in order to overcome innate and acquired resistance to these drugs and thus expand the array of cancers that could benefit from them. We show that human cancer cell lines which respond poorly to ABT-888 (a PARPi), become sensitive to it when co-treated with vorinostat (a histone deacetylase inhibitor (HDACi)). Vorinostat also sensitized PARPis insensitive cancer cell lines to 6-thioguanine (6-TG)–a drug that targets PARPis sensitive cells. The sensitizing effect of vorinostat was associated with increased phosphorylation of eukaryotic initiation factor (eIF) 2α which in and of itself increases the sensitivity of cancer cells to ABT-888. Importantly, these drug combinations did not affect survival of normal fibroblasts and breast cells, and significantly increased the inhibition of xenograft tumor growth relative to each drug alone, without affecting the mice weight or their liver and kidney function. Our results show that combination of vorinostat and ABT-888 could potentially prove useful for treatment of cancer with innate resistance to PARPis due to active HRR machinery, while the combination of vorinostat and 6-TG could potentially overcome innate or acquired resistance to PARPis due to secondary or reversal BRCA mutations, to decreased PARP-1 level or to increased expression of multiple drug resistant proteins. Importantly, drugs which increase phosphorylation of eIF2α may mimic the sensitizing effect of vorinostat on cellular response to PARPis or to 6-TG, without activating all of its downstream effectors.

show abstract

“…It is presumed that the liposomal formulation caused damage to erythrocytes, which accelerated their removal by macrophages in the spleen. [37] To assess acute toxicity, we performed hemograms and a blood biochemical analysis for the liver, renal, and muscle parameters in Balb/c mice after the administration of frequent dosages of aldox-NFP, aldox, and Doxil (2.5 mg kg −1 of drug content three times a week). None of the three treatments changed the number and morphology of the blood cells (Figure 8b).…”

Section: Resultsmentioning

confidence: 99%

Functional Peptide Nanofibers with Unique Tumor Targeting and Enzyme‐Induced Local Retention Properties

Bellat

Ting

Southard

et al. 2018

Adv Funct Materials

View full text Add to dashboard Cite

An effective tumoral delivery system should show minimal removal by the reticuloendothelial system (RES), promote tumor uptake and penetration, and minimize on-site clearance. This study reports the design and synthesis of advanced self-assembling peptide nanofiber precursor (NFP) analogues. The peptidic nature of NFP offers the design flexibility for on-demand customization with imaging agents and surface charges while maintaining a set size, allowing for real-time monitoring of kinetic and dynamic tumoral delivery by multimodal fluorescence/positron emission tomography/computed tomography (fluo/PET/CT) imaging, for formulation optimization. The optimized glutathione (GSH)-NFP displays a reduced capture by the RES as well as excellent tumor targeting and tissue invasion properties compared to naive NFP. Inside a tumor, GSH-NFP can structurally transform into ten times larger interfibril networks, serving as in situ depot that promotes weeks-long local retention. This nanofiber, which can further be designed to release the active pharmacophores within a tumor microenvironment, displays a superior therapeutic efficacy for inhibiting disease progression and improving the survival of animals bearing triple-negative breast cancer tumors compared to free drug and liposome formulation of the drug, in addition to a favorable toxicity profile.

show abstract

Specific Hemosiderin Deposition in Spleen Induced by a Low Dose of Cisplatin: Altered Iron Metabolism and Its Implication as an Acute Hemosiderin Formation Model

Cited by 47 publications

References 41 publications

Cinnamic Acid and Cinnamaldehyde Ameliorate Cisplatin-Induced Splenotoxicity in Rats

Cinnamic Acid and Cinnamaldehyde Ameliorate Cisplatin-Induced Splenotoxicity in Rats

Overcoming Resistance of Cancer Cells to PARP-1 Inhibitors with Three Different Drug Combinations

Functional Peptide Nanofibers with Unique Tumor Targeting and Enzyme‐Induced Local Retention Properties

Contact Info

Product

Resources

About