Role of Zinc in Human Islet Amyloid Polypeptide Aggregation

Brender, Jeffrey R.; Hartman, Kevin; Nanga, Ravi Prakash Reddy; Popovych, Nataliya; Bea, Roberto de la Salud; Vivekanandan, Subramanian; Marsh, E. Neil G.; Ramamoorthy, Ayyalusamy

doi:10.1021/ja1007867

Cited by 216 publications

(284 citation statements)

References 91 publications

(199 reference statements)

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“…However, under normal conditions it is likely that the granule peptides also have influences on each other. Interaction in vitro of insulin, c-peptide, proinsulin and zinc with hIAPP have been investigated and shown to have variable effects on IAPP fibrillogenesis; high concentrations of zinc accelerate, but lower concentrations reduce fibril formation (Westermark et al 1996, Brender et al 2010. Human proinsulin and insulin formed heteromolecular complexes with hIAPP and prevented fibrillogenesis (Jaikaran et al 2004, Larson & Miranker 2004, Knight et al 2008, Wiltzius et al 2009).…”

Section: Proiapp/iapp In Granulesmentioning

confidence: 99%

The β-cell assassin: IAPP cytotoxicity

Raleigh

Zhang

Hastoy

et al. 2017

Journal of Molecular Endocrinology

102

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Islet amyloid polypeptide (IAPP) forms cytotoxic oligomers and amyloid fibrils in islets in type 2 diabetes (T2DM). The causal factors for amyloid formation are largely unknown. Mechanisms of molecular folding and assembly of human IAPP (hIAPP) into β-sheets, oligomers and fibrils have been assessed by detailed biophysical studies of hIAPP and non-fibrillogenic, rodent IAPP (rIAPP); cytotoxicity is associated with the early phases (oligomers/multimers) of fibrillogenesis. Interaction with synthetic membranes promotes β-sheet assembly possibly via a transient α-helical molecular conformation. Cellular hIAPP cytotoxicity can be activated from intracellular or extracellular sites. In transgenic rodents overexpressing hIAPP, intracellular pro-apoptotic signals can be generated at different points in β-cell protein synthesis. Increased cellular trafficking of proIAPP, failure of the unfolded protein response (UPR) or excess trafficking of misfolded peptide via the degradation pathways can induce apoptosis; these data indicate that defects in intracellular handling of hIAPP can induce cytotoxicity. However, there is no evidence for IAPP overexpression in T2DM. Extracellular amyloidosis is directly related to the degree of β-cell apoptosis in islets in T2DM. IAPP fragments, fibrils and multimers interact with membranes causing disruption in vivo and in vitro. These findings support a role for extracellular IAPP in β-sheet conformation in cytotoxicity. Inhibitors of fibrillogenesis are useful tools to determine the aberrant mechanisms that result in hIAPP molecular refolding and islet amyloidosis. However, currently, their role as therapeutic agents remains uncertain.

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Section: Proiapp/iapp In Granulesmentioning

confidence: 99%

The β-cell assassin: IAPP cytotoxicity

Raleigh

Zhang

Hastoy

et al. 2017

Journal of Molecular Endocrinology

102

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“…One possible reason for this observation could be that it might take a longer time for the hIAPP molecules to form aggregates than the time needed for the Langmuir monolayer experiment. It typically took a few hours to detect fibril formation by thioflavin T fluorescence in solution [27,32,34], but one set of Langmuir monolayer experiments needed only 30-40 min. Another possibility could be that some aggregation did form, but the surface pressure-area isotherm could not detect it.…”

Section: The Ph Effect On the Hiapp Langmuir Monolayermentioning

confidence: 99%

Human islet amyloid polypeptide at the air–aqueous interface: a Langmuir monolayer approach

Mićić

Orbulescu

et al. 2012

J. R. Soc. Interface.

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Human islet amyloid polypeptide (hIAPP) is the source of the major component of the amyloid deposits found in the islets of Langerhans of around 95 per cent type 2 diabetic patients. The formation of aggregates and mature fibrils is thought to be responsible for the dysfunction and death of the insulin-producing pancreatic b-cells. Investigation on the conformation, orientation and self-assembly of the hIAPP at time zero could be beneficial for our understanding of its stability and aggregation process. To obtain these insights, the hIAPP at time zero was studied at the air-aqueous interface using the Langmuir monolayer technique. The properties of the hIAPP Langmuir monolayer at the air -aqueous interface on a NaCl subphase with pH 2.0, 5.6 and 9.0 were examined by surface pressure-and potential-area isotherms, UV-Vis absorption, fluorescence spectroscopy and Brewster angle microscopy. The conformational and orientational changes of the hIAPP Langmuir monolayer under different surface pressures were characterized by p-polarized infrared-reflection absorption spectroscopy, and the results did not show any prominent changes of conformation or orientation. The predominant secondary structure of the hIAPP at the air -aqueous interface was a-helix conformation, with a parallel orientation to the interface during compression. These results showed that the hIAPP Langmuir monolayer at the air -aqueous interface was stable, and no aggregate or domain of the hIAPP at the air -aqueous interface was observed during the time of experiments.

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“…Zn plays a key role in the storage and secretion of insulin, which then increases the uptake of glucose (Kazi et al, 2008;Rungby, 2010). The decreased plasma level of Zn adversely affects the ability of islet cells to produce and secrete insulin (Brender et al, 2010;Rungby, 2010). The Zn transporter (ZnT8) is a key protein for the regulation of insulin secretion from the pancreatic β-cells.…”

Section: Cumentioning

confidence: 99%

Role of heavy metals in human health and particularly in respect to diabetic patients

Asif¹

2017

TANG [HUMANITAS MEDICINE]

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Minerals are individual of the components of foods and are not produced in the body but essential for best possible health. Several essential metals are vital for the appropriate performance of various enzymes, transcriptional factors and proteins that are essential in various biochemical paths. Metals like zinc (Zn), magnesium (Mg), and manganese (Mn) are cofactors of hundreds of enzymes. Zn is involved in the synthesis and secretion of insulin from the pancreatic β-cells. Chromium (Cr) increases the insulin receptors activity on target tissues, mainly in muscle cells. Insulin hormone is required to maintain the blood glucose amount in normal range. Continual increase of blood serum glucose level leads to marked chronic hyperglycemia or diabetes mellitus. Deficiency of insulin or its resistance, blood glucose level exceeds the upper limit of the common range of 126 mg/dl. Poor glucose control and diabetes changes the levels of essential trace elements such as Zn, Mg, Mn, Cr, iron etc. by rising urinary excretion and their related decrease in the blood. The aim of this article to discusses the important roles of essential trace elements in particular perspective of type 2 diabetes.

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Role of Zinc in Human Islet Amyloid Polypeptide Aggregation

Cited by 216 publications

References 91 publications

The β-cell assassin: IAPP cytotoxicity

The β-cell assassin: IAPP cytotoxicity

Human islet amyloid polypeptide at the air–aqueous interface: a Langmuir monolayer approach

Role of heavy metals in human health and particularly in respect to diabetic patients

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