Your search keyword '"chemical entities"' showing total 34 results

1. The Pharmaceutical Industry in 2023: An Analysis of FDA Drug Approvals from the Perspective of Molecules.

Author

de la Torre, Beatriz G. and Albericio, Fernando

Subjects

*DRUG approval, *SMALL molecules, *DRUG analysis, *ANTIBODY-drug conjugates, *OLIGONUCLEOTIDES, *PEPTIDES

Abstract

With the COVID-19 pandemic behind us, the U.S. Food and Drug Administration (FDA) has approved 55 new drugs in 2023, a figure consistent with the number authorized in the last five years (53 per year on average). Thus, 2023 marks the second-best yearly FDA harvest after 2018 (59 approvals) in all the series. Monoclonal antibodies (mAbs) continue to be the class of drugs with the most approvals, with an exceptional 12, a number that makes it the most outstanding year for this class. As in 2022, five proteins/enzymes have been approved in 2023. However, no antibody–drug conjugates (ADCs) have been released onto the market. With respect to TIDES (peptides and oligonucleotides), 2023 has proved a spectacular year, with a total of nine approvals, corresponding to five peptides and four oligonucleotides. Natural products continue to be the best source of inspiration for drug development, with 10 new products on the market. Three drugs in this year's harvest are pegylated, which may indicate the return of pegylation as a method to increase the half-lives of drugs after the withdrawal of peginesatide from the market in 2013. Following the trends in recent years, two bispecific drugs have been authorized in 2023. As in the preceding years, fluorine and/or N-aromatic heterocycles are present in most of the drugs. Herein, the 55 new drugs approved by the FDA in 2023 are analyzed exclusively on the basis of their chemical structure. They are classified as the following: biologics (antibodies, proteins/enzymes); TIDES (peptide and oligonucleotides); combined drugs; pegylated drugs; natural products; nitrogen aromatic heterocycles; fluorine-containing molecules; and other small molecules. [ABSTRACT FROM AUTHOR]

Published

2024

2. The Pharmaceutical Industry in 2023: An Analysis of FDA Drug Approvals from the Perspective of Molecules

Author

Beatriz G. de la Torre and Fernando Albericio

Subjects

antibodies, biologics, chemical entities, fluorine-based drugs, imaging, natural products, Organic chemistry, QD241-441

Abstract

With the COVID-19 pandemic behind us, the U.S. Food and Drug Administration (FDA) has approved 55 new drugs in 2023, a figure consistent with the number authorized in the last five years (53 per year on average). Thus, 2023 marks the second-best yearly FDA harvest after 2018 (59 approvals) in all the series. Monoclonal antibodies (mAbs) continue to be the class of drugs with the most approvals, with an exceptional 12, a number that makes it the most outstanding year for this class. As in 2022, five proteins/enzymes have been approved in 2023. However, no antibody–drug conjugates (ADCs) have been released onto the market. With respect to TIDES (peptides and oligonucleotides), 2023 has proved a spectacular year, with a total of nine approvals, corresponding to five peptides and four oligonucleotides. Natural products continue to be the best source of inspiration for drug development, with 10 new products on the market. Three drugs in this year’s harvest are pegylated, which may indicate the return of pegylation as a method to increase the half-lives of drugs after the withdrawal of peginesatide from the market in 2013. Following the trends in recent years, two bispecific drugs have been authorized in 2023. As in the preceding years, fluorine and/or N-aromatic heterocycles are present in most of the drugs. Herein, the 55 new drugs approved by the FDA in 2023 are analyzed exclusively on the basis of their chemical structure. They are classified as the following: biologics (antibodies, proteins/enzymes); TIDES (peptide and oligonucleotides); combined drugs; pegylated drugs; natural products; nitrogen aromatic heterocycles; fluorine-containing molecules; and other small molecules.

Published

2024

3. The Pharmaceutical Industry in 2022: An Analysis of FDA Drug Approvals from the Perspective of Molecules.

Author

de la Torre, Beatriz G. and Albericio, Fernando

Subjects

*DRUG approval, *SMALL molecules, *DRUG analysis, *OLIGONUCLEOTIDES, *COVID-19 pandemic, *ANTIBODY-drug conjugates, *MONOCLONAL antibodies

Abstract

While 2021 ended with the world engulfed in the COVID-19 Omicron wave, 2022 has ended in almost all countries, except China, with COVID-19 being likened to the flu. In this context, the U.S. Food and Drug Administration (FDA) has authorized only 37 new drugs this year compared to an average of 52 in the last four years. Thus 2022 is the second lowest harvest after 2016 in the last six years. This ranking may be transient and will be confirmed in the coming years. In this regard, the reduction in the number of drugs accepted by the FDA this year applies only to the so-called small molecules as there has been no variation in the respective numbers of biologics or TIDES (peptides and oligonucleotides). Monoclonal antibodies (mAbs) continue to be the class with the most drugs authorized (9), while proteins/enzymes (5) and an antibody–drug conjugate complete the biologics harvest. In 2022, five TIDES and seven drugs inspired by natural products have received the green light, thus showing the same tendency as in previous years. Finally, pharmaceutical agents with nitrogen aromatic heterocycles and/or fluorine atoms continue to be predominant among small molecules this year. Furthermore, three drugs have been approved for imaging, reinforcing the trend in recent years for this class of treatments. A keyword in 2022 is bispecificity since four drugs have this property (two mAbs, one protein, and one peptide). Herein, the 37 new drugs approved by the FDA in 2022 are analyzed. On the basis of chemical structure alone, these drugs are classified as the following: biologics (antibodies, antibody-drug conjugates, proteins/enzymes), TIDES (peptide and oligonucleotides), combined drugs, natural products; nitrogen aromatic heterocycles, fluorine-containing molecules, and other small molecules. [ABSTRACT FROM AUTHOR]

Published

2023

4. Biomolecules Versus Smaller Chemicals in Toxicology: ICH, EU, and US Recommendations

Author

Ruthsatz, Manfred, Chiavaroli, Carlo, Cassar, M. A., Voisin, Emmanuelle M., Reichl, Franz-Xaver, editor, and Schwenk, Michael, editor

Published

2021

5. The Pharmaceutical Industry in 2022: An Analysis of FDA Drug Approvals from the Perspective of Molecules

Author

Beatriz G. de la Torre and Fernando Albericio

Subjects

antibodies, biologics, chemical entities, fluorine-based drugs, imaging, natural products, Organic chemistry, QD241-441

Abstract

While 2021 ended with the world engulfed in the COVID-19 Omicron wave, 2022 has ended in almost all countries, except China, with COVID-19 being likened to the flu. In this context, the U.S. Food and Drug Administration (FDA) has authorized only 37 new drugs this year compared to an average of 52 in the last four years. Thus 2022 is the second lowest harvest after 2016 in the last six years. This ranking may be transient and will be confirmed in the coming years. In this regard, the reduction in the number of drugs accepted by the FDA this year applies only to the so-called small molecules as there has been no variation in the respective numbers of biologics or TIDES (peptides and oligonucleotides). Monoclonal antibodies (mAbs) continue to be the class with the most drugs authorized (9), while proteins/enzymes (5) and an antibody–drug conjugate complete the biologics harvest. In 2022, five TIDES and seven drugs inspired by natural products have received the green light, thus showing the same tendency as in previous years. Finally, pharmaceutical agents with nitrogen aromatic heterocycles and/or fluorine atoms continue to be predominant among small molecules this year. Furthermore, three drugs have been approved for imaging, reinforcing the trend in recent years for this class of treatments. A keyword in 2022 is bispecificity since four drugs have this property (two mAbs, one protein, and one peptide). Herein, the 37 new drugs approved by the FDA in 2022 are analyzed. On the basis of chemical structure alone, these drugs are classified as the following: biologics (antibodies, antibody-drug conjugates, proteins/enzymes), TIDES (peptide and oligonucleotides), combined drugs, natural products; nitrogen aromatic heterocycles, fluorine-containing molecules, and other small molecules.

Published

2023

6. E-Code Checker Application

Author

Kasim, Shahreen, Azahar, Ummi Aznazirah, Samsudin, Noor Azah, Fudzee, Mohd Farhan Md, Mahdin, Hairulnizam, Ramli, Azizul Azhar, Suparjoh, Suriawati, Kacprzyk, Janusz, Series Editor, Pal, Nikhil R., Advisory Editor, Bello Perez, Rafael, Advisory Editor, Corchado, Emilio S., Advisory Editor, Hagras, Hani, Advisory Editor, Kóczy, László T., Advisory Editor, Kreinovich, Vladik, Advisory Editor, Lin, Chin-Teng, Advisory Editor, Lu, Jie, Advisory Editor, Melin, Patricia, Advisory Editor, Nedjah, Nadia, Advisory Editor, Nguyen, Ngoc Thanh, Advisory Editor, Wang, Jun, Advisory Editor, Herawan, Tutut, editor, Ghazali, Rozaida, editor, Nawi, Nazri Mohd, editor, and Deris, Mustafa Mat, editor

Published

2017

7. A Review of African Medicinal and Aromatic Plants

Author

Van Wyk, Ben-Erik, Máthé, Ákos, Series editor, Neffati, Mohamed, editor, and Najjaa, Hanen, editor

Published

2017

8. About continuity and rupture in the history of chemistry: the fourth chemical revolution (1945–1966).

Author

Chamizo, José A.

Subjects

*SCIENTIFIC community, *HISTORY of chemistry, *REVOLUTIONS, *ARTICLES of incorporation, *CONTINUITY, *CHEMISTRY

Abstract

A layered interpretation of the history of chemistry is discussed through chemical revolutions. A chemical revolution (or rupture, discontinuity, transition) mainly by emplacement, instead of replacement, procedures were identified by: a radical reinterpretation of existing thought recognized by contemporaries themselves, which means the appearance of new concepts and the arrival of new theories; the use of new instruments changed the way in which its practitioners looked and worked in the world and through exemplars, new entities were discovered or incorporated; the opening of new subdisciplines, which produced, separated scientific communities. The fourth chemical revolution, fundamentally characterized by the incorporation of new instruments in chemical practices is discussed. [ABSTRACT FROM AUTHOR]

Published

2019

9. The Pharmaceutical Industry in 2019. An Analysis of FDA Drug Approvals from the Perspective of Molecules

Author

Beatriz G. de la Torre and Fernando Albericio

Subjects

antibodies, antibody drug conjugate, api, biologics, chemical entities, drug discovery, fluorine-based drugs, natural products, oligonucleotides, peptides, pyrazoles, tides, small molecules, Organic chemistry, QD241-441

Abstract

During 2019, the US Food and Drug Administration (FDA) approved 48 new drugs (38 New Chemical Entities and 10 Biologics). Although this figure is slightly lower than that registered in 2018 (59 divided between 42 New Chemical Entities and 17 Biologics), a year that broke a record with respect to new drugs approved by this agency, it builds on the trend initiated in 2017, when 46 drugs were approved. Of note, three antibody drug conjugates, three peptides, and two oligonucleotides were approved in 2019. This report analyzes the 48 new drugs of the class of 2019 from a strictly chemical perspective. The classification, which was carried out on the basis of chemical structure, includes the following: Biologics (antibody drug conjugates, antibodies, and proteins); TIDES (peptide and oligonucleotides); drug combinations; natural products; and small molecules.

Published

2020

10. The Pharmaceutical Industry in 2017. An Analysis of FDA Drug Approvals from the Perspective of Molecules.

Author

de la Torre, Beatriz G. and Albericio, Fernando

Subjects

*DRUG approval, *PHARMACEUTICAL policy, *DRUG development, *BIOLOGICALS, *SMALL molecules, *INDUSTRIES, *PHARMACEUTICAL industry, *GOVERNMENT policy

Abstract

This is an analysis from a chemical point of view of the 46 drugs (34 New Chemical Entities and 12 Biologics) approved by the FDA during 2017. The drugs included in the 2017 "harvest" have been classified on the basis of their chemical structure: biologics (antibodies and proteins); peptides; amino acids and natural products; drug combinations; and small molecules. [ABSTRACT FROM AUTHOR]

Published

2018

11. The Pharmaceutical Industry in 2021. An Analysis of FDA Drug Approvals from the Perspective of Molecules

Author

de la Torre, Beatriz G., Albericio, Fernando, de la Torre, Beatriz G., and Albericio, Fernando

Abstract

Similar to last year, 2021 will be remembered for the COVID-19 pandemic. Although five vaccines have been approved by the two most important drug regulatory agencies, namely the US Food and Drug Administration (FDA) and the European Medicines Agency (EMA), the pandemic has still not been brought under control. However, despite the context of a global pandemic, 2021 has been an excellent year with respect to drug approvals by the FDA. In 2021, 50 drugs have been authorized, making it the fourth-best year after 2018 (59 drugs) and 1996 and 2020 (53 each). Regarding biologics, 2021 has been the third-best year to date, with 14 approvals, and it has also witnessed the authorization of 36 small molecules. Of note, nine peptides, eight monoclonal antibodies, two antibody-drug conjugates, and two oligonucleotides have been approved this year. From them, five of the molecules are pegylated and three of them highly pegylated. The presence of nitrogen aromatic heterocycles and/or fluorine atoms are once again predominant among the so-called small molecules. This report analyzes the 50 new drugs approved in 2021 from a chemical perspective, as it did for those authorized in the previous five years. On the basis of chemical structure alone, the drugs that received approval in 2021 are classified as the following: biologics (antibodies, antibody-drug conjugates, enzymes, and pegylated proteins); TIDES (peptide and oligonucleotides); combined drugs; natural products; nitrogen aromatic heterocycles; fluorine-containing molecules; and other small molecules.

Published

2022

12. The Pharmaceutical Industry in 2018. An Analysis of FDA Drug Approvals from the Perspective of Molecules

Author

Beatriz G. de la Torre and Fernando Albericio

Subjects

antibodies, API, biologics, chemical entities, drug discovery, fluorine based drugs, natural products, oligonucleotides, peptide, TIDES, small molecules, Organic chemistry, QD241-441

Abstract

The Food and Drug Administration approved 59 new drugs (42 New Chemical Entities and 17 Biologics) during 2018. This number breaks the previous record of 53 approved by the same organization in 1996. The 17 new biologics approved in 2018 also represent an important milestone for this kind of drug and they clearly exceed the 12 approved in 2015 and 2017. Herein, the 59 new drugs of the class of 2018 are analyzed from a strictly chemical perspective. The classification has been carried out on the basis of the chemical structure and includes the following: Biologics (antibodies and enzymes); TIDES (peptides and oligonucleotides) and natural products; drug combinations; and small molecules.

Published

2019

13. The Pharmaceutical Industry in 2016. An Analysis of FDA Drug Approvals from a Perspective of the Molecule Type.

Author

de la Torre, Beatriz G. and Albericio, Fernando

Subjects

*DRUG approval, *PHARMACEUTICAL industry, *CHEMICAL structure, *SMALL molecules

Abstract

This is an analysis from a chemical point of view of the 22 drugs accepted by the FDA during 2016. The different drugs from the 2016 "harvest" have been classified according to their chemical structure: antibodies; TIDES (oligonucleotides and peptides); amino acids and natural products; drug combination; and small molecules. [ABSTRACT FROM AUTHOR]

Published

2017

14. The Pharmaceutical Industry in 2021. An Analysis of FDA Drug Approvals from the Perspective of Molecules

Author

Fernando Albericio and Beatriz G. De la Torre

Subjects

Drug Industry, TIDES, Oligonucleotides, Pharmaceutical Science, Organic chemistry, Biologics, History, 21st Century, Antibodies, Analytical Chemistry, antibody-drug conjugate, QD241-441, antibodies, Humans, biologics, Physical and Theoretical Chemistry, Antibody-drug conjugate, fluorine-based drugs, Drug Approval, Natural products, Biological Products, Drug discovery, CBER, United States Food and Drug Administration, CDER, COVID-19, Pegylation, United States, Nitrogen aromatic heterocycles, Chemistry (miscellaneous), API, Molecular Medicine, Chemical entities, Peptides

Abstract

Similar to last year, 2021 will be remembered for the COVID-19 pandemic. Although five vaccines have been approved by the two most important drug regulatory agencies, namely the US Food and Drug Administration (FDA) and the European Medicines Agency (EMA), the pandemic has still not been brought under control. However, despite the context of a global pandemic, 2021 has been an excellent year with respect to drug approvals by the FDA. In 2021, 50 drugs have been authorized, making it the fourth-best year after 2018 (59 drugs) and 1996 and 2020 (53 each). Regarding biologics, 2021 has been the third-best year to date, with 14 approvals, and it has also witnessed the authorization of 36 small molecules. Of note, nine peptides, eight monoclonal antibodies, two antibody-drug conjugates, and two oligonucleotides have been approved this year. From them, five of the molecules are pegylated and three of them highly pegylated. The presence of nitrogen aromatic heterocycles and/or fluorine atoms are once again predominant among the so-called small molecules. This report analyzes the 50 new drugs approved in 2021 from a chemical perspective, as it did for those authorized in the previous five years. On the basis of chemical structure alone, the drugs that received approval in 2021 are classified as the following: biologics (antibodies, antibody-drug conjugates, enzymes, and pegylated proteins); TIDES (peptide and oligonucleotides); combined drugs; natural products; nitrogen aromatic heterocycles; fluorine-containing molecules; and other small molecules., The work performed by the authors laboratory is funded by the National Research Foundation (NRF) and the University of KwaZulu-Natal.

Published

2022

15. The Pharmaceutical Industry in 2017. An Analysis of FDA Drug Approvals from the Perspective of Molecules

Author

Beatriz G. de la Torre and Fernando Albericio

Subjects

drug discovery, API, peptide, biologics, small molecules, chemical entities, Organic chemistry, QD241-441

Abstract

This is an analysis from a chemical point of view of the 46 drugs (34 New Chemical Entities and 12 Biologics) approved by the FDA during 2017. The drugs included in the 2017 “harvest” have been classified on the basis of their chemical structure: biologics (antibodies and proteins); peptides; amino acids and natural products; drug combinations; and small molecules.

Published

2018

16. The Pharmaceutical Industry in 2020. An Analysis of FDA Drug Approvals from the Perspective of Molecules

Author

National Research Foundation (South Africa), University of KwaZulu-Natal, de la Torre, Beatriz G., Albericio, Fernando, National Research Foundation (South Africa), University of KwaZulu-Natal, de la Torre, Beatriz G., and Albericio, Fernando

Abstract

Although the pharmaceutical industry will remember 2020 as the year of COVID-19, it is important to highlight that this year has been the second-best—together with 1996—in terms of the number of drugs accepted by the US Food and Drug Administration (FDA). Each of these two years witnessed the authorization of 53 drugs—a number surpassed only in 2018 with 59 pharmaceutical agents. The 53 approvals in 2020 are divided between 40 new chemical entities and 13 biologic drugs (biologics). Of note, ten monoclonal antibodies, two antibody–drug conjugates, three peptides, and two oligonucleotides have been approved in 2020. Close inspection of the so-called small molecules reveals the significant presence of fluorine atoms and/or nitrogen aromatic heterocycles. This report analyzes the 53 new drugs of the 2020 harvest from a strictly chemical perspective, as it did for those authorized in the previous four years. On the basis of chemical structure alone, the drugs that received approval in 2020 are classified as the following: biologics (antibodies, antibody-drug conjugates, and proteins); TIDES (peptide and oligonucleotides); natural products; fluorine-containing molecules; nitrogen aromatic heterocycles; and other small molecules

Published

2021

17. The Pharmaceutical Industry in 2016. An Analysis of FDA Drug Approvals from a Perspective of the Molecule Type

Author

Beatriz G. de la Torre and Fernando Albericio

Subjects

drug discovery, API, peptide, biologics, small molecules, chemical entities, Organic chemistry, QD241-441

Abstract

This is an analysis from a chemical point of view of the 22 drugs accepted by the FDA during 2016. The different drugs from the 2016 “harvest” have been classified according to their chemical structure: antibodies; TIDES (oligonucleotides and peptides); amino acids and natural products; drug combination; and small molecules.

Published

2017

18. The Pharmaceutical Industry in 2020. An Analysis of FDA Drug Approvals from the Perspective of Molecules

Author

Fernando Albericio, Beatriz G. De la Torre, National Research Foundation (South Africa), and University of KwaZulu-Natal

Subjects

Drug Industry, natural products, TIDES, Oligonucleotides, Pharmaceutical Science, Review, Biologics, History, 21st Century, Antibodies, Analytical Chemistry, lcsh:QD241-441, lcsh:Organic chemistry, Drug Discovery, antibodies, biologics, Physical and Theoretical Chemistry, fluorine-based drugs, Drug Approval, chemical entities, Natural products, oligonucleotides, Fluorine-based drugs, United States Food and Drug Administration, CBER, Drug discovery, Organic Chemistry, CDER, Small molecules, antibody–drug conjugate, COVID-19, United States, Nitrogen aromatic heterocycles, small molecules, Chemistry (miscellaneous), API, peptides, Molecular Medicine, Chemical entities, nitrogen aromatic heterocycles, Peptides, Antibody–drug conjugate

Abstract

Although the pharmaceutical industry will remember 2020 as the year of COVID-19, it is important to highlight that this year has been the second-best—together with 1996—in terms of the number of drugs accepted by the US Food and Drug Administration (FDA). Each of these two years witnessed the authorization of 53 drugs—a number surpassed only in 2018 with 59 pharmaceutical agents. The 53 approvals in 2020 are divided between 40 new chemical entities and 13 biologic drugs (biologics). Of note, ten monoclonal antibodies, two antibody–drug conjugates, three peptides, and two oligonucleotides have been approved in 2020. Close inspection of the so-called small molecules reveals the significant presence of fluorine atoms and/or nitrogen aromatic heterocycles. This report analyzes the 53 new drugs of the 2020 harvest from a strictly chemical perspective, as it did for those authorized in the previous four years. On the basis of chemical structure alone, the drugs that received approval in 2020 are classified as the following: biologics (antibodies, antibody-drug conjugates, and proteins); TIDES (peptide and oligonucleotides); natural products; fluorine-containing molecules; nitrogen aromatic heterocycles; and other small molecules, The work performed by the authors is funded by the National Research Foundation (NRF) and the University of KwaZulu-Natal.

Published

2021

19. Pharmaceutical nanoparticle isolation using CO2-assisted dynamic bed coating

Author

Luis Padrela, Kevin M. Ryan, Vivek Verma, and SFI

Subjects

Active ingredient, Materials science, Pharmaceutical Science, Nanoparticle, 02 engineering and technology, engineering.material, 021001 nanoscience & nanotechnology, 030226 pharmacology & pharmacy, Supercritical fluid, Microcrystalline cellulose, 03 medical and health sciences, chemistry.chemical_compound, 0302 clinical medicine, Coating, chemistry, Chemical engineering, Spray drying, engineering, Solubility, 0210 nano-technology, Dissolution, chemical entities, CO2 spray

Abstract

peer-reviewed Poor solubility of new chemical entities (NCEs) is a major bottleneck in the pharmaceutical industry which typically leads to poor drug bioavailability and efficacy. Nanotechnologies offer an interesting route to improve the apparent solubility and dissolution rate of pharmaceutical drugs, and processes such as nano-spray drying and supercritical CO2-assisted spray drying (SASD) provide a route to engineer and produce solid drug nanoparticles. However, dried nanoparticles often show poor rheological properties (e.g. flowability, tabletability) and their isolation using these methods is typically inefficient and leads to poor collection yields. The work presented herein demonstrates a novel production and isolation method for drug nanoparticles using a ‘top spray dynamic bed coating’ process, which uses CO2 spray as the fluidizing gas. Nanoparticles of three BCS class II Active Pharmaceutical Ingredients (APIs), namely carbamazepine (CBZ), ketoprofen (KET) and risperidone (RIS), were produced and successfully coated onto micron-sized microcrystalline cellulose (MCC) particles. The size distribution of the API nanoparticles was in the range of 90–490 nm. The stable forms of CBZ (form III), KET (form I), and the metastable form of RIS (form B) were produced and coated onto MCC carrier microparticles. All the isolated solids presented optimal rheological properties along with a 2–6 fold improvement in the dissolution rate of the corresponding APIs. Hence, the ‘top spray dynamic bed coater’ developed in this work demonstrates to be an efficient approach to produce and coat API nanoparticles onto carrier particles with optimal rheological properties and improved dissolution.

Published

2021

20. Chemical named entities recognition: a review on approaches and applications.

Author

Eltyeb, Safaa and Salim, Naomie

Subjects

*ELECTRONIC information resources, *INFORMATION resources, *DIGITAL libraries, *CHEMINFORMATICS, *CHEMISTRY, *COMPUTERS, *INFORMATION science

Abstract

The rapid increase in the flow rate of published digital information in all disciplines has resulted in a pressing need for techniques that can simplify the use of this information. The chemistry literature is very rich with information about chemical entities. Extracting molecules and their related properties and activities from the scientific literature to "text mine" these extracted data and determine contextual relationships helps research scientists, particularly those in drug development. One of the most important challenges in chemical text mining is the recognition of chemical entities mentioned in the texts. In this review, the authors briefly introduce the fundamental concepts of chemical literature mining, the textual contents of chemical documents, and the methods of naming chemicals in documents. We sketch out dictionary-based, rule-based and machine learning, as well as hybrid chemical named entity recognition approaches with their applied solutions. We end with an outlook on the pros and cons of these approaches and the types of chemical entities extracted. [ABSTRACT FROM AUTHOR]

Published

2014

21. The Pharmaceutical Industry in 2019. An Analysis of FDA Drug Approvals from the Perspective of Molecules

Author

Fernando Albericio and Beatriz G. De la Torre

Subjects

Immunoconjugates, Drug Industry, natural products, TIDES, Oligonucleotides, Pharmaceutical Science, Review, History, 21st Century, Analytical Chemistry, drug discovery, lcsh:QD241-441, 03 medical and health sciences, Structure-Activity Relationship, 0302 clinical medicine, lcsh:Organic chemistry, Humans, antibodies, biologics, Physical and Theoretical Chemistry, Drug Approval, fluorine-based drugs, chemical entities, 030304 developmental biology, 0303 health sciences, Biological Products, Molecular Structure, United States Food and Drug Administration, Organic Chemistry, Antibodies, Monoclonal, Drugs, Investigational, United States, pyrazoles, Drug Combinations, small molecules, Chemistry (miscellaneous), 030220 oncology & carcinogenesis, API, peptides, Molecular Medicine, antibody drug conjugate

Abstract

During 2019, the US Food and Drug Administration (FDA) approved 48 new drugs (38 New Chemical Entities and 10 Biologics). Although this figure is slightly lower than that registered in 2018 (59 divided between 42 New Chemical Entities and 17 Biologics), a year that broke a record with respect to new drugs approved by this agency, it builds on the trend initiated in 2017, when 46 drugs were approved. Of note, three antibody drug conjugates, three peptides, and two oligonucleotides were approved in 2019. This report analyzes the 48 new drugs of the class of 2019 from a strictly chemical perspective. The classification, which was carried out on the basis of chemical structure, includes the following: Biologics (antibody drug conjugates, antibodies, and proteins); TIDES (peptide and oligonucleotides); drug combinations; natural products; and small molecules.

Published

2020

22. Fluorescence readouts in HTS: no gain without pain?

Author

Gribbon, Philip and Sewing, Andreas

Subjects

*FLUORESCENCE, *BIOLOGICAL reagents, *BIOLOGICAL assay, *CHEMICAL reagents, *RADIOACTIVITY

Abstract

Fluorescence-based detection technologies are frequently applied in biological testing, due to their unique advantages in setting up homogeneous, sensitive assays in miniaturized formats. However, the wide application of these readouts has highlighted challenges in reagent design and problems with interference from biological reagents and compounds. Here, we summarize the current application of fluorescence-based detection methodologies, focusing on the problems faced by assay developers and on solutions to reduce false positive and negative results in fluorescence-based HTS. [Copyright &y& Elsevier]

Published

2003

23. The Pharmaceutical Industry in 2018. An Analysis of FDA Drug Approvals from the Perspective of Molecules

Author

Fernando Albericio and Beatriz G. De la Torre

Subjects

0301 basic medicine, Drug Industry, natural products, TIDES, Pharmaceutical Science, Review, Antibodies, Analytical Chemistry, drug discovery, lcsh:QD241-441, 03 medical and health sciences, 0302 clinical medicine, lcsh:Organic chemistry, Humans, biologics, Physical and Theoretical Chemistry, Drug Approval, chemical entities, Biological Products, oligonucleotides, Molecular Structure, United States Food and Drug Administration, Organic Chemistry, peptide, United States, small molecules, 030104 developmental biology, Pharmaceutical Preparations, Chemistry (miscellaneous), 030220 oncology & carcinogenesis, API, fluorine based drugs, Molecular Medicine

Abstract

The Food and Drug Administration approved 59 new drugs (42 New Chemical Entities and 17 Biologics) during 2018. This number breaks the previous record of 53 approved by the same organization in 1996. The 17 new biologics approved in 2018 also represent an important milestone for this kind of drug and they clearly exceed the 12 approved in 2015 and 2017. Herein, the 59 new drugs of the class of 2018 are analyzed from a strictly chemical perspective. The classification has been carried out on the basis of the chemical structure and includes the following: Biologics (antibodies and enzymes); TIDES (peptides and oligonucleotides) and natural products; drug combinations; and small molecules.

Published

2019

24. The Pharmaceutical Industry in 2021. An Analysis of FDA Drug Approvals from the Perspective of Molecules.

Author

de la Torre BG and Albericio F

Subjects

Biological Products, History, 21st Century, Humans, United States, Drug Approval history, Drug Approval statistics & numerical data, Drug Industry history, United States Food and Drug Administration

Abstract

Similar to last year, 2021 will be remembered for the COVID-19 pandemic. Although five vaccines have been approved by the two most important drug regulatory agencies, namely the US Food and Drug Administration (FDA) and the European Medicines Agency (EMA), the pandemic has still not been brought under control. However, despite the context of a global pandemic, 2021 has been an excellent year with respect to drug approvals by the FDA. In 2021, 50 drugs have been authorized, making it the fourth-best year after 2018 (59 drugs) and 1996 and 2020 (53 each). Regarding biologics, 2021 has been the third-best year to date, with 14 approvals, and it has also witnessed the authorization of 36 small molecules. Of note, nine peptides, eight monoclonal antibodies, two antibody-drug conjugates, and two oligonucleotides have been approved this year. From them, five of the molecules are pegylated and three of them highly pegylated. The presence of nitrogen aromatic heterocycles and/or fluorine atoms are once again predominant among the so-called small molecules. This report analyzes the 50 new drugs approved in 2021 from a chemical perspective, as it did for those authorized in the previous five years. On the basis of chemical structure alone, the drugs that received approval in 2021 are classified as the following: biologics (antibodies, antibody-drug conjugates, enzymes, and pegylated proteins); TIDES (peptide and oligonucleotides); combined drugs; natural products; nitrogen aromatic heterocycles; fluorine-containing molecules; and other small molecules.

Published

2022

25. The Pharmaceutical Industry in 2020. An Analysis of FDA Drug Approvals from the Perspective of Molecules.

Author

de la Torre, Beatriz G., Albericio, Fernando, and Muñoz-Torrero, Diego

Subjects

*DRUG approval, *OLIGONUCLEOTIDES, *SMALL molecules, *DRUG analysis, *ANTIBODY-drug conjugates, *MOLECULES

Abstract

Although the pharmaceutical industry will remember 2020 as the year of COVID-19, it is important to highlight that this year has been the second-best—together with 1996—in terms of the number of drugs accepted by the US Food and Drug Administration (FDA). Each of these two years witnessed the authorization of 53 drugs—a number surpassed only in 2018 with 59 pharmaceutical agents. The 53 approvals in 2020 are divided between 40 new chemical entities and 13 biologic drugs (biologics). Of note, ten monoclonal antibodies, two antibody–drug conjugates, three peptides, and two oligonucleotides have been approved in 2020. Close inspection of the so-called small molecules reveals the significant presence of fluorine atoms and/or nitrogen aromatic heterocycles. This report analyzes the 53 new drugs of the 2020 harvest from a strictly chemical perspective, as it did for those authorized in the previous four years. On the basis of chemical structure alone, the drugs that received approval in 2020 are classified as the following: biologics (antibodies, antibody-drug conjugates, and proteins); TIDES (peptide and oligonucleotides); natural products; fluorine-containing molecules; nitrogen aromatic heterocycles; and other small molecules. [ABSTRACT FROM AUTHOR]

Published

2021

26. The Pharmaceutical Industry in 2016. An Analysis of FDA Drug Approvals from a Perspective of the Molecules

Author

Fernando Albericio and Beatriz G. De la Torre

Subjects

0301 basic medicine, Farmacologia, Drug Industry, Databases, Pharmaceutical, Pharmaceutical Science, Review, Antibodies, Drug design, Analytical Chemistry, drug discovery, Small Molecule Libraries, lcsh:QD241-441, 03 medical and health sciences, 0302 clinical medicine, lcsh:Organic chemistry, Humans, biologics, Amino Acids, Physical and Theoretical Chemistry, Drug Approval, chemical entities, Pharmacology, Biological Products, Disseny de medicaments, Molecular Structure, United States Food and Drug Administration, Organic Chemistry, United States, peptide, small molecules, 030104 developmental biology, Pharmaceutical Preparations, Chemistry (miscellaneous), 030220 oncology & carcinogenesis, API, Molecular Medicine, Pèptids, Peptides

Abstract

This is an analysis from a chemical point of view of the 22 drugs accepted by the FDA during 2016. The different drugs from the 2016 "harvest" have been classified according to their chemical structure: antibodies; TIDES (oligonucleotides and peptides); amino acids and natural products; drug combination; and small molecules.

Published

2017

27. The Pharmaceutical Industry in 2019. An Analysis of FDA Drug Approvals from the Perspective of Molecules.

Author

de la Torre, Beatriz G. and Albericio, Fernando

Subjects

*DRUG approval, *DRUG analysis, *SMALL molecules, *PHARMACEUTICAL industry, *MOLECULES

Abstract

During 2019, the US Food and Drug Administration (FDA) approved 48 new drugs (38 New Chemical Entities and 10 Biologics). Although this figure is slightly lower than that registered in 2018 (59 divided between 42 New Chemical Entities and 17 Biologics), a year that broke a record with respect to new drugs approved by this agency, it builds on the trend initiated in 2017, when 46 drugs were approved. Of note, three antibody drug conjugates, three peptides, and two oligonucleotides were approved in 2019. This report analyzes the 48 new drugs of the class of 2019 from a strictly chemical perspective. The classification, which was carried out on the basis of chemical structure, includes the following: Biologics (antibody drug conjugates, antibodies, and proteins); TIDES (peptide and oligonucleotides); drug combinations; natural products; and small molecules. [ABSTRACT FROM AUTHOR]

Published

2020

28. The Pharmaceutical Industry in 2020. An Analysis of FDA Drug Approvals from the Perspective of Molecules.

Author

Torre BG and Albericio F

Subjects

History, 21st Century, United States, Drug Approval legislation & jurisprudence, Drug Industry, United States Food and Drug Administration legislation & jurisprudence

Abstract

Although the pharmaceutical industry will remember 2020 as the year of COVID-19, it is important to highlight that this year has been the second-best-together with 1996-in terms of the number of drugs accepted by the US Food and Drug Administration (FDA). Each of these two years witnessed the authorization of 53 drugs-a number surpassed only in 2018 with 59 pharmaceutical agents. The 53 approvals in 2020 are divided between 40 new chemical entities and 13 biologic drugs (biologics). Of note, ten monoclonal antibodies, two antibody-drug conjugates, three peptides, and two oligonucleotides have been approved in 2020. Close inspection of the so-called small molecules reveals the significant presence of fluorine atoms and/or nitrogen aromatic heterocycles. This report analyzes the 53 new drugs of the 2020 harvest from a strictly chemical perspective, as it did for those authorized in the previous four years. On the basis of chemical structure alone, the drugs that received approval in 2020 are classified as the following: biologics (antibodies, antibody-drug conjugates, and proteins); TIDES (peptide and oligonucleotides); natural products; fluorine-containing molecules; nitrogen aromatic heterocycles; and other small molecules., Competing Interests: The authors declare no conflict of interest.

Published

2021

29. The Pharmaceutical Industry in 2018. An Analysis of FDA Drug Approvals from the Perspective of Molecules.

Author

G. de la Torre, Beatriz, Albericio, Fernando, and Muñoz-Torrero, Diego

Subjects

*BIOLOGICALS, *DRUGS, *IMMUNOGLOBULINS, *ENZYMES

Abstract

The Food and Drug Administration approved 59 new drugs (42 New Chemical Entities and 17 Biologics) during 2018. This number breaks the previous record of 53 approved by the same organization in 1996. The 17 new biologics approved in 2018 also represent an important milestone for this kind of drug and they clearly exceed the 12 approved in 2015 and 2017. Herein, the 59 new drugs of the class of 2018 are analyzed from a strictly chemical perspective. The classification has been carried out on the basis of the chemical structure and includes the following: Biologics (antibodies and enzymes); TIDES (peptides and oligonucleotides) and natural products; drug combinations; and small molecules. [ABSTRACT FROM AUTHOR]

Published

2019

30. The Application of the Open Pharmacological Concepts Triple Store (Open PHACTS) to Support Drug Discovery Research

Author

Joseline Ratnam, Edgar Jacoby, José Brea, Ronny Siebes, Hannah Tipney, María Isabel Loza, Lars Richter, Chris T. Evelo, Jean-Marc Neefs, Andra Waagmeester, Glyn Bradley, Christine Chichester, Chau Han Chau, Gerhard F. Ecker, Emiliano Cuadrado-Rodriguez, Daniela Digles, Barbara Zdrazil, Stefan Senger, Bioinformatica, and RS: NUTRIM - R4 - Gene-environment interaction

Subjects

Interoperability, BIOLOGICAL INTEREST, lcsh:Medicine, PROTEIN, Drug research and development, Bioinformatics, Database and Informatics Methods, 0302 clinical medicine, HYP MICE, Protein kinases, Medicine and Health Sciences, Use case, Vitamin D, lcsh:Science, 0303 health sciences, Multidisciplinary, Drug discovery, GENE ONTOLOGY, COLON-CANCER, 3. Good health, Chemistry, Identification (information), Databases as Topic, 030220 oncology & carcinogenesis, Physical Sciences, Information Retrieval, Gene ontologies, DOPAMINE-RECEPTORS, Research Article, CHEMICAL ENTITIES, Process (engineering), DATABASE, Biological Data Management, Biology, Research and Analysis Methods, 03 medical and health sciences, Calcitriol, Relevance (information retrieval), Semantic Web, 1,25-DIHYDROXYVITAMIN D-3, 030304 developmental biology, Pharmacology, lcsh:R, Biology and Life Sciences, Computational Biology, Data science, Database searching, VITAMIN-D-RECEPTOR, Biological Databases, Workflow, Open Source Drug Discovery, 25-DIHYDROXYVITAMIN D-3, lcsh:Q, Medicinal Chemistry, Software

Abstract

Integration of open access, curated, high-quality information from multiple disciplines in the Life and Biomedical Sciences provides a holistic understanding of the domain. Additionally, the effective linking of diverse data sources can unearth hidden relationships and guide potential research strategies. However, given the lack of consistency between descriptors and identifiers used in different resources and the absence of a simple mechanism to link them, gathering and combining relevant, comprehensive information from diverse databases remains a challenge. The Open Pharmacological Concepts Triple Store (Open PHACTS) is an Innovative Medicines Initiative project that uses semantic web technology approaches to enable scientists to easily access and process data from multiple sources to solve real-world drug discovery problems. The project draws together sources of publicly-available pharmacological, physicochemical and biomolecular data, represents it in a stable infrastructure and provides well-defined information exploration and retrieval methods. Here, we highlight the utility of this platform in conjunction with workflow tools to solve pharmacological research questions that require interoperability between target, compound, and pathway data. Use cases presented herein cover 1) the comprehensive identification of chemical matter for a dopamine receptor drug discovery program 2) the identification of compounds active against all targets in the Epidermal growth factor receptor (ErbB) signaling pathway that have a relevance to disease and 3) the evaluation of established targets in the Vitamin D metabolism pathway to aid novel Vitamin D analogue design. The example workflows presented illustrate how the Open PHACTS Discovery Platform can be used to exploit existing knowledge and generate new hypotheses in the process of drug discovery.

Published

2014

31. Databases on food phytochemicals and their health-promoting effects

Author

Claudine Manach, Mireia Urpi-Sarda, Cristina Andres-Lacueva, Paul A. Kroon, Masanori Arita, David S. Wishart, Augustin Scalbert, International Agency for Research on Cancer (IARC), University of Barcelona, The University of Tokyo (UTokyo), Institute of Food Research, Unité de Nutrition Humaine (UNH), Institut National de la Recherche Agronomique (INRA)-Université d'Auvergne - Clermont-Ferrand I (UdA)-Clermont Université, and University of Alberta

Subjects

CHEMICAL ENTITIES, databases, Databases, Factual, 030309 nutrition & dietetics, BIOCYC COLLECTION, [SDV]Life Sciences [q-bio], METABOLIC PATHWAYS, BIOLOGICAL INTEREST, METACYC DATABASE, Health Promotion, Biology, computer.software_genre, Field (computer science), 03 medical and health sciences, foods, nutrigenomics, Biological property, Animals, Humans, Health food, 030304 developmental biology, 2. Zero hunger, 0303 health sciences, Database, Plant Extracts, PATHWAY/GENOME DATABASES, health, General Chemistry, MASS-SPECTROMETRY, bioinformatics, phytochemicals, POLYPHENOL INTAKE, CONTROLLED-TRIALS, Nutrigenomics, POSTMENOPAUSAL WOMEN, Dietary Phytochemicals, Plants, Edible, General Agricultural and Biological Sciences, computer, metabolism, Nutritive Value

Abstract

International audience; Considerable information on the chemistry and biological properties of dietary phytochemicals has accumulated over the past three decades. The scattering of the data in tens of thousands publications and the diversity of experimental approaches and reporting formats all make the exploitation of this information very difficult. Some of the data have been collected and stored in electronic databases so that they can be automatically updated and retrieved. These databases will be particularly important in the evaluation of the effects on health of phytochemicals and in facilitating the exploitation of nutrigenomic data. The content of over 50 databases on chemical structures, spectra, metabolic pathways in plants, occurrence and concentrations in foods, metabolism in humans and animals, biological properties, and effects on health or surrogate markers of health is reviewed. Limits of these databases are emphasized, and needs and recommendations for future developments are underscored. More investments in the construction of databases on phytochemicals and their effects on health are clearly needed. They should greatly contribute to the success of future research in this field.

Published

2011

32. Chemical named entities recognition: a review on approaches and applications

Author

Safaa Eltyeb and Naomie Salim

Subjects

Information retrieval, Information extraction, Computer science, Chemical nomenclature, Scientific literature, Review, Library and Information Sciences, computer.software_genre, Chemical names, Data science, Computer Graphics and Computer-Aided Design, Sketch, Computer Science Applications, Named-entity recognition, Chemical entities, Physical and Theoretical Chemistry, computer

Abstract

The rapid increase in the flow rate of published digital information in all disciplines has resulted in a pressing need for techniques that can simplify the use of this information. The chemistry literature is very rich with information about chemical entities. Extracting molecules and their related properties and activities from the scientific literature to “text mine” these extracted data and determine contextual relationships helps research scientists, particularly those in drug development. One of the most important challenges in chemical text mining is the recognition of chemical entities mentioned in the texts. In this review, the authors briefly introduce the fundamental concepts of chemical literature mining, the textual contents of chemical documents, and the methods of naming chemicals in documents. We sketch out dictionary-based, rule-based and machine learning, as well as hybrid chemical named entity recognition approaches with their applied solutions. We end with an outlook on the pros and cons of these approaches and the types of chemical entities extracted.

Published

2014

33. The Pharmaceutical Industry in 2016. An Analysis of FDA Drug Approvals from a Perspective of the Molecule Type.

Author

Torre BG and Albericio F

Subjects

Amino Acids chemistry, Antibodies chemistry, Databases, Pharmaceutical statistics & numerical data, Drug Industry, Humans, Molecular Structure, Small Molecule Libraries chemistry, United States, United States Food and Drug Administration, Biological Products chemistry, Drug Approval, Pharmaceutical Preparations chemistry

Abstract

This is an analysis from a chemical point of view of the 22 drugs accepted by the FDA during 2016. The different drugs from the 2016 "harvest" have been classified according to their chemical structure: antibodies; TIDES (oligonucleotides and peptides); amino acids and natural products; drug combination; and small molecules.

Published

2017

34. Pharmaceutical nanoparticle isolation using CO2-assisted dynamic bed coating

Author

SFI, Verma, Vivek, Ryan, Kevin M., Padrela, Luis, SFI, Verma, Vivek, Ryan, Kevin M., and Padrela, Luis

Abstract

peer-reviewed, Poor solubility of new chemical entities (NCEs) is a major bottleneck in the pharmaceutical industry which typically leads to poor drug bioavailability and efficacy. Nanotechnologies offer an interesting route to improve the apparent solubility and dissolution rate of pharmaceutical drugs, and processes such as nano-spray drying and supercritical CO2-assisted spray drying (SASD) provide a route to engineer and produce solid drug nanoparticles. However, dried nanoparticles often show poor rheological properties (e.g. flowability, tabletability) and their isolation using these methods is typically inefficient and leads to poor collection yields. The work presented herein demonstrates a novel production and isolation method for drug nanoparticles using a ‘top spray dynamic bed coating’ process, which uses CO2 spray as the fluidizing gas. Nanoparticles of three BCS class II Active Pharmaceutical Ingredients (APIs), namely carbamazepine (CBZ), ketoprofen (KET) and risperidone (RIS), were produced and successfully coated onto micron-sized microcrystalline cellulose (MCC) particles. The size distribution of the API nanoparticles was in the range of 90–490 nm. The stable forms of CBZ (form III), KET (form I), and the metastable form of RIS (form B) were produced and coated onto MCC carrier microparticles. All the isolated solids presented optimal rheological properties along with a 2–6 fold improvement in the dissolution rate of the corresponding APIs. Hence, the ‘top spray dynamic bed coater’ developed in this work demonstrates to be an efficient approach to produce and coat API nanoparticles onto carrier particles with optimal rheological properties and improved dissolution.