A Novel Tool for Detecting Amyloid Deposits in Systemic Amyloidosis In Vitro and In Vivo

Ando, Yumiko; Haraoka, Katsuki; Terazaki, Hisayasu; Tanoue, Yutaka; Ishikawa, Kazuo; Katsuragi, Shoichi; Nakamura, Masaaki; Sun, Xuguo; Nakagawa, Kazuko; Sasamoto, Kazumi; Takesako, Kazuhiro; Ishizaki, Takashi; Sasaki, Yutaka; Doh‐ura, Katsumi

doi:10.1097/01.lab.0000101701.87433.c5

Cited by 20 publications

(10 citation statements)

References 48 publications

(87 reference statements)

Supporting

Mentioning

Contrasting

Order By: Relevance

“…Although amyloid deposits are usually identified by means of CR staining, our histopathological studies showed that venous EFEMP1 amyloid deposits had faint CR staining. In contrast, these venous EFEMP1 amyloid deposits were confirmed by electron microscopy and were clearly detected by FSB fluorescent staining, which is reportedly a more sensitive method than CR staining to detect various kinds of amyloid deposits . We should note, therefore, that CR staining may be not sufficient to detect venous EFEMP1 amyloid deposits and may sometimes lead to misdiagnosis of EFEMP1 amyloidosis, so more sensitive methods, such as FSB staining and immunohistochemical staining, are preferred for a more accurate diagnosis of venous EFEMP1 amyloidosis.…”

Section: Discussionmentioning

confidence: 91%

A novel age‐related venous amyloidosis derived from EGF‐containing fibulin‐like extracellular matrix protein 1

Tasaki

Ueda

Hoshii

et al. 2018

The Journal of Pathology

Self Cite

View full text Add to dashboard Cite

Most intractable tissue‐degenerative disorders share a common pathogenic condition, so‐called proteinopathy. Amyloid‐related disorders are the most common proteinopathies and are characterized by amyloid fibril deposits in the brain or other organs. Aging is generally associated with the development of these amyloid‐related disorders, but we still do not fully understand how functional proteins become pathogenic amyloid deposits during the human aging process. We identified a novel amyloidogenic protein, named epidermal growth factor‐containing fibulin‐like extracellular matrix protein 1 (EFEMP1), in massive venous amyloid deposits in specimens that we obtained from an autopsied patient who died of gastrointestinal bleeding. Our postmortem analyses of additional patients indicate that EFEMP1 amyloid deposits frequently developed in systemic venous walls of elderly people. EFEMP1 was highly expressed in veins, and aging enhanced venous EFEMP1 expression. In addition, biochemical analyses indicated that these venous amyloid deposits consisted of C‐terminal regions of EFEMP1. In vitro studies showed that C‐terminal regions formed amyloid fibrils, which inhibited venous tube formation and cell viability. EFEMP1 thus caused a novel age‐related venous amyloid‐related disorder frequently found in the elderly population. Understanding EFEMP1 amyloid formation provides new insights into amyloid‐related disorders occurring during the aging process. Copyright © 2018 Pathological Society of Great Britain and Ireland. Published by John Wiley & Sons, Ltd.

show abstract

Section: Discussionmentioning

confidence: 91%

A novel age‐related venous amyloidosis derived from EGF‐containing fibulin‐like extracellular matrix protein 1

Tasaki

Ueda

Hoshii

et al. 2018

The Journal of Pathology

Self Cite

View full text Add to dashboard Cite

show abstract

“…A fluorescent derivative of Congo Red, (trans, trans)-1-bromo-2,5-bis-(3-hydroxycarbonyl-4-hydroxy)styrylbenzene (BSB), has also been employed for the detection of amyloid deposits in tissue sections [19]. With an emission maximum of 520 nm, this probe offers improved performance with respect to the avoidance of background associated with intrinsic and fixative-induced autofluorescence in cells and tissues.…”

Section: Discussionmentioning

confidence: 99%

Novel Cell- and Tissue-Based Assays for Detecting Misfolded and Aggregated Protein Accumulation Within Aggresomes and Inclusion Bodies

Shen

Coleman

Chan

et al. 2010

Cell Biochem Biophys

186

185

View full text Add to dashboard Cite

Aggresomes and related inclusion bodies appear to serve as storage depots for misfolded and aggregated proteins within cells, which can potentially be degraded by the autophagy pathway. A homogenous fluorescence-based assay was devised to detect aggregated proteins inside aggresomes and inclusion bodies within an authentic cellular context. The assay employs a novel red fluorescent molecular rotor dye, which is essentially nonfluorescent until it binds to structural features associated with the aggregated protein cargo. Aggresomes and related structures were generated within cultured cells using various potent, cell permeable, proteasome inhibitors: MG-132, lactacystin, epoxomicin and bortezomib, and then selectively detected with the fluorescent probe. Employing the probe in combination with various fluorescein-labeled primary antibodies facilitated co-localization of key components of the autophagy system (ubiquitin, p62, and LC3) with aggregated protein cargo by fluorescence microscopy. Furthermore, cytoplasmic aggregates were highlighted in SK-N-SH human neuroblastoma cells incubated with exogenously supplied amyloid beta peptide 1–42. SMER28, a small molecule modulator of autophagy acting via an mTOR-independent mechanism, prevented the accumulation of amyloid beta peptide within these cells. The described assay allows assessment of the effects of protein aggregation directly in cells, without resorting to the use of non-physiological protein mutations or genetically engineered cell lines. With minor modification, the assay was also adapted to the analysis of frozen or formalin-fixed, paraffin-embedded tissue sections, with demonstration of co-localization of aggregated cargo with β-amyloid and tau proteins in brain tissue sections from Alzheimer’s disease patients.

show abstract

“…In the patients with small amyloid deposits, repeated biopsies should be required to confirm the diagnosis. In addition to the commonly used Congo red staining, (E,E)-1-bromo-2,5-bis-(3-hydroxycarbonyl-4-hydroxy) styrylbenzene (BSB) and (E,E)-1-fluoro-2,5-bis-(3-hydroxycarbonyl-4-hydroxy) styrylbenzene (FSB) can be employed to detect a small amount of amyloid deposits in biopsy specimens, because these two chemical agents bind to amyloid fibrils more strongly than Congo red [49,50].…”

Section: Histopathological Analysesmentioning

confidence: 99%

Diagnosis and Therapeutic Approaches to Transthyretin Amyloidosis

Ando

Ueda

2012

CMC

View full text Add to dashboard Cite

Hereditary amyloidogenic transthyretin (TTR) (ATTR) amyloidosis is an autosomal dominant form of fatal hereditary amyloidosis. Owing to progress in biochemical and molecular genetic analyses, this disease is now believed to occur worldwide. As of today, reports of about 120 different points of single or double mutations, or a deletion in the TTR gene have been reported, and several different phenotypes of ATTR amyloidosis have been documented. In addition, since liver transplantation has been established to halt the progression of hereditary ATTR amyloidosis in the early stage, rapid and reliable diagnostic system for ATTR amyloidosis is needed. On the other hand, senile systemic amyloidosis (SSA) derived from wild-type (WT) TTR affects primarily in the heart and lungs and occasionally in carpal ligaments in the elderly. To perform accurate diagnosis and effective treatments, we should distinguish between hereditary ATTR amyloidosis and SSA by means of genetic and proteomic analyses. The liver transplantation for hereditary ATTR amyloidosis has become a well-established treatment, because the main source of serum variant TTR is shut out. However, this treatment has several problems, such as expensive medical costs, lifelong administration of immunosuppressants, non-indication for the mutated-TTR gene carriers without clinical symptoms, shortage of liver donors, and further development of cardiac and ocular disorders. Therefore, we and other ATTR amyloidosis research groups have been investigating the possibility of stabilization of variant TTR, gene therapy, and immunotherapy for ATTR amyloidosis on the basis of TTR amyloid formation mechanism. We present here the current diagnostic procedure and therapeutic approaches for the disease.

show abstract

A Novel Tool for Detecting Amyloid Deposits in Systemic Amyloidosis In Vitro and In Vivo

Cited by 20 publications

References 48 publications

A novel age‐related venous amyloidosis derived from EGF‐containing fibulin‐like extracellular matrix protein 1

A novel age‐related venous amyloidosis derived from EGF‐containing fibulin‐like extracellular matrix protein 1

Novel Cell- and Tissue-Based Assays for Detecting Misfolded and Aggregated Protein Accumulation Within Aggresomes and Inclusion Bodies

Diagnosis and Therapeutic Approaches to Transthyretin Amyloidosis

Contact Info

Product

Resources

About