Camelid Single-Domain Antibodies: Historical Perspective and Future Outlook

Arbabi‐Ghahroudi, Mehdi

doi:10.3389/fimmu.2017.01589

Cited by 159 publications

(127 citation statements)

References 103 publications

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“…The first strategy would be to employ either a small receptor-binding domain (RBD) or a neutralizing antibody targeting the ACE-2 receptor, thus blocking the binding of S protein and preventing virus entry into cells. Initial in vitro results have shown promising results [67,68] and specific monoclonal antibodies are being contemplated as candidates for treatment [69,70]. The main limitation of using RBDs or antibodies is that the treatment must be given within a specific time window, before the initiation of viral replication [20].…”

Section: Treatmentmentioning

confidence: 99%

SARS-CoV-2 and Coronavirus Disease 2019: What We Know So Far

et al. 2020

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In December 2019, a cluster of fatal pneumonia cases presented in Wuhan, China. They were caused by a previously unknown coronavirus. All patients had been associated with the Wuhan Wholefood market, where seafood and live animals are sold. The virus spread rapidly and public health authorities in China initiated a containment effort. However, by that time, travelers had carried the virus to many countries, sparking memories of the previous coronavirus epidemics, severe acute respiratory syndrome (SARS) and Middle East respiratory syndrome (MERS), and causing widespread media attention and panic. Based on clinical criteria and available serological and molecular information, the new disease was called coronavirus disease of 2019 , and the novel coronavirus was called SARS Coronavirus-2 (SARS-CoV-2), emphasizing its close relationship to the 2002 SARS virus (SARS-CoV). The scientific community raced to uncover the origin of the virus, understand the pathogenesis of the disease, develop treatment options, define the risk factors, and work on vaccine development. Here we present a summary of current knowledge regarding the novel coronavirus and the disease it causes.

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Section: Treatmentmentioning

confidence: 99%

SARS-CoV-2 and Coronavirus Disease 2019: What We Know So Far

et al. 2020

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“…Given the many challenges, discovery and preclinical validation of novel immune targets with limited expression on normal human tissues is only the first step, even when utilizing modern omics techniques. Specific antibody clones can be rapidly identified using human IgG transgenic animals, human phage libraries, or humanized single VH domain libraries (35). These antibody binding domains can then be reshaped into chimeric receptors, multivalent and/or multispecific formats for diagnostic and therapeutic applications.…”

Section: Future Strategies Of Antibody-based Therapies: a Reassessmentmentioning

confidence: 99%

Immunotherapy of Pediatric Solid Tumors: Treatments at a Crossroads, with an Emphasis on Antibodies

Casey

Cheung

2020

Cancer Immunology Research

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Over the last decade, immunotherapy has rapidly changed the therapeutic landscape and prognosis for many hematologic malignancies and adult solid tumors. Despite this success, immunotherapy for pediatric solid tumors remains in the early stages of development, and significant clinical benefit has yet to be realized, with anti-GD2 for neuroblastoma being the exception. The limited neoepitope expression and paucity of T-cell infiltration into the immunosuppressive tumor microenvironment have hampered current established immunotherapies. Emerging approaches to recruit T cells, to convert phenotypically "cold" into "inflamed" tumors, and to vastly improve therapeutic indices hold exceptional promise. Here, we review these approaches, highlighting the role of the tumor microenvironment and novel antibody platforms to maximize the full clinical potential of immunotherapy in pediatric oncology.

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“…This is the most recent addition to the fragment-based class of format. Single-domain antibodies are derived from immunoglobulins that contain a single variable domain, which are found naturally in some camelids (camels, llamas, alpacas and vicuñas) [ 80 ] and cartilaginous fishes (i.e., sharks) [ 81 ]. The single-domain antibodies from camelids are known as V H H or nanobodies, whereas the ones from sharks are known as V-NAR (variable new antigen receptor domain) (Fig.…”

Section: Fragment-based Bispecific Antibodiesmentioning

confidence: 99%

Expanding the Boundaries of Biotherapeutics with Bispecific Antibodies

Husain¹,

Ellerman²

2018

BioDrugs

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Bispecific antibodies have moved from being an academic curiosity with therapeutic promise to reality, with two molecules being currently commercialized (Hemlibra® and Blincyto®) and many more in clinical trials. The success of bispecific antibodies is mainly due to the continuously growing number of mechanisms of actions (MOA) they enable that are not accessible to monoclonal antibodies. One of the earliest MOA of bispecific antibodies and currently the one with the largest number of clinical trials is the redirecting of the cytotoxic activity of T-cells for oncology applications, now extending its use in infective diseases. The use of bispecific antibodies for crossing the blood–brain barrier is another important application because of its potential to advance the therapeutic options for neurological diseases. Another noteworthy application due to its growing trend is enabling a more tissue-specific delivery or activity of antibodies. The different molecular solutions to the initial hurdles that limited the development of bispecific antibodies have led to the current diverse set of bispecific or multispecific antibody formats that can be grouped into three main categories: IgG-like formats, antibody fragment-based formats, or appended IgG formats. The expanded applications of bispecific antibodies come at the price of additional challenges for clinical development. The rising complexity in their structure may increase the risk of immunogenicity and the multiple antigen specificity complicates the selection of relevant species for safety assessment.

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Camelid Single-Domain Antibodies: Historical Perspective and Future Outlook

Cited by 159 publications

References 103 publications

SARS-CoV-2 and Coronavirus Disease 2019: What We Know So Far

SARS-CoV-2 and Coronavirus Disease 2019: What We Know So Far

Immunotherapy of Pediatric Solid Tumors: Treatments at a Crossroads, with an Emphasis on Antibodies

Expanding the Boundaries of Biotherapeutics with Bispecific Antibodies

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