Novel Drug Delivery System to Bone Using Acidic Oligopeptide: Pharmacokinetic Characteristics and Pharmacological Potential

Sekido, Tohru; Sakura, Naoki; Higashi, Yasuhiko; Miya, Kazuhiro; Nitta, Youko; Nomura, Masatoshi; Sawanishi, Hiroyuki; Morito, Keiko; Masamune, Yukito; Kasugai, Shohei; Yokogawa, Koiçhi; Miyamoto, K

doi:10.3109/10611860108997922

Cited by 67 publications

(70 citation statements)

References 15 publications

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“…The uptake level in soft tissues was less than in estradiol. Thus, estradiol with at least six residues of L-Asp was observed to prevent bone loss in ovariectomized (osteoporosis) mice without causing liver damage or increasing uterine weight [61]. Bone density improved with fewer adverse effects, suggesting that estradiol tagged with the acidic oligopeptide is a potential drug to treat a postmenopausal osteoporosis [43].…”

Section: Discussionmentioning

confidence: 96%

Enhancement of drug delivery to bone: Characterization of human tissue-nonspecific alkaline phosphatase tagged with an acidic oligopeptide

Nishioka

Tomatsu

Gutiérrez

et al. 2006

Molecular Genetics and Metabolism

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Hypophosphatasia is caused by deficiency of activity of the tissue-nonspecific alkaline phosphatase (TNSALP), resulting in a defect of bone mineralization. Enzyme replacement therapy (ERT) with partially purified plasma enzyme was attempted but with little clinical improvement. Attaining clinical effectiveness with ERT for hypophosphatasia may require delivering functional TNSALP enzyme to bone. We tagged the C-terminal-anchorless TNSALP enzyme with an acidic oligopeptide (a six or eight residue stretch of L-Asp), and compared the biochemical properties of the purified tagged and untagged enzymes derived from Chinese hamster ovary cell lines. The specific activities of the purified enzymes tagged with the acidic oligopeptide were the same as the untagged enzyme. In vitro affinity experiments showed the tagged enzymes had 30-fold higher affinity for hydroxyapatite than the untagged enzyme. Lectin affinity chromatography for carbohydrate structure showed little difference among the three enzymes. Biodistribution pattern from single infusion of the fluorescence-labeled enzymes into mice showed delayed clearance from the plasma up to 18h post infusion and the amount of tagged enzyme retained in bone was 4-fold greater than that of the untagged enzyme. In vitro mineralization assays with the bone marrow from a hypophosphatasia patient using each of the three enzymes in the presence of high concentrations of pyrophosphate provided evidence of bone mineralization. These results show the anchorless enzymes tagged with an acidic oligopeptide are delivered efficiently to bone and function bioactively in bone mineralization, at least in vitro. They suggest potential advantages for use of these tagged enzymes in ERT for hypophosphatasia, which should be explored.

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Section: Discussionmentioning

confidence: 96%

Enhancement of drug delivery to bone: Characterization of human tissue-nonspecific alkaline phosphatase tagged with an acidic oligopeptide

Nishioka

Tomatsu

Gutiérrez

et al. 2006

Molecular Genetics and Metabolism

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“…A drug attached to HA is released during bone resorption processes and targeting a drug to HA is a potential strategy for a selective drug delivery to bone [73,74]. Kasugai et al, 2000 showed that they could enhance estradiol uptake by bone and prevent osteoporosis by tagging the hormone to Glu 6 (E6) [75,76]. We and others have recently applied this new bone-targeting system to a large molecule, an enzyme (tissue nonspecific alkaline phosphatase), showing that the tagged enzymes are delivered more efficiently to bone [77][78][79] and that the tagged enzyme improves clinical and pathological effects of a mouse model of a systemic bone disease, hypophosphatasia, better than untagged native enzyme [80].…”

Section: Long Circulating Ert-a Chemically Modified β-Glucuronidase (mentioning

confidence: 99%

Therapies for the bone in mucopolysaccharidoses

Tomatsu

Barrera

Alméciga-Díaz

et al. 2015

Molecular Genetics and Metabolism

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Patients with mucopolysaccharidoses (MPS) have accumulation of glycosaminoglycans in multiple tissues which may cause coarse facial features, mental retardation, recurrent ear and nose infections, inguinal and umbilical hernias, hepatosplenomegaly, and skeletal deformities. Clinical features related to bone lesions may include marked short stature, cervical stenosis, pectus carinatum, small lungs, joint rigidity (but laxity for MPS IV), kyphoscoliosis, lumbar gibbus, and genu valgum. Patients with MPS are often wheelchair-bound and physical handicaps increase with age as a result of progressive skeletal dysplasia, abnormal joint mobility, and osteoarthritis, leading to 1) stenosis of the upper cervical region, 2) restrictive small lung, 3) hip dysplasia, 4) restriction of joint movement, and 5) surgical complications. Patients often need multiple orthopedic procedures including cervical decompression and fusion, carpal tunnel release, hip reconstruction and replacement, and femoral or tibial osteotomy through their lifetime. Current measures to intervene in bone disease progression are not perfect and palliative, and improved therapies are urgently required.Enzyme replacement therapy (ERT), hematopoietic stem cell transplantation (HSCT), and gene therapy are available or in development for some types of MPS. Delivery of sufficient enzyme to bone, especially avascular cartilage, to prevent or ameliorate the devastating skeletal dysplasias remains an unmet challenge. The use of an anti-inflammatory drug is also under clinical study. Therapies should start at a very early stage prior to irreversible bone lesion, and damage since the severity of skeletal dysplasia is associated with level of activity during daily life.This review illustrates a current overview of therapies and their impact for bone lesions in MPS including ERT, HSCT, gene therapy, and anti-inflammatory drugs.

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“…The 3-carboxylate and 4-carbonyl groups in quinolone are known to be responsible for potential chelating property with divalent metals such as calcium existing in bone, and these groups remain intact in NFLX-D 6 , but not in LVFX-D 6 (32). It is also known that the extension of the number of acidic amino acid increases the bone accumulating property of acidic oligopeptide in vivo (21). Thus, it was hypothesized that the intact 3-carboxylate and 4-carbonyl groups in NFLX-D 6 further augmented the affinity of L-Asp hexapeptide to bone.…”

Section: Discussionmentioning

confidence: 97%

“…To determine the binding affinity of acidic oligopeptides to hydroxyapatite, homopeptides consisting of two to ten residues of acidic amino acids were conjugated with 9-fluorenylmethylchloroformate and the binding affinities were investigated in vitro. The results indicated that the dissociation constants of the acidic oligopeptides decreased with increasing numbers of acidic amino acid residues, and the maximal binding rates reached a plateau at six residues, which were independent of acidic amino acid specie (Asp or Glu) and optical isomeric form (L or D) (21). In vivo, fluorescein-labeled L-Asp hexapeptide accumulated specifically in bone at 24 h after systemic administration in mice and was not detected in other tissues.…”

Section: Introductionmentioning

confidence: 89%