News

In October, we added 115 citations in DIDB, including 55 in vitro (with 23 articles published in October 2024) and 60 in vivo articles (with 35 articles published in October 2024).

3 NDA/BLAs approved in 2024, including lebrikizumab (EBGLYSS), levacetylleucine (AQNEURSA), and flurpiridaz F18 (FLYRCADO) were also curated in DIDB.

You can check the citations that are recently published and entered in DIDB and all the NDAs/BLAs in DIDB.

As always, feel free to contact us if you have any questions or comments.

The DDI Marker Studies Knowledgebase has been updated in October 2024 and is available in the DIDB Resource Center.

Our Editorial Team has dedicated effort on identifying substrates and perpetrators of UGT enzymes. More than 30 UGT substrates, inhibitors, and inducers recommended by the ICH M12 DDI guideline have been added to the knowledgebase with supporting DDI and/or PGx evidence. In addition, we have continued to identify substrates and inhibitors for renal transporters by reviewing all the existing data. Overall, 65 compounds have been identified as substates, inhibitors, and inducers of CYPs, UGTs, and various transporters, including P-gp, BCRP, OATP1B1, OATP1B3, OAT1, OAT3, OCT2, MATE1, and MATE2-K. Notably, one compound was classified as a sensitive substrate of CYP1A2 and one as a strong inhibitor of CYP3A based on PBPK data (AUCR > 10), which could potentially lead to significant drug interactions mediated by these CYPs.

To view a comprehensive list of additions and modifications, including new compounds and updates to existing entries, you may use the “Recent Update” column (Column AE) on the spreadsheet and select “yes.”

In addition to substrates, inhibitors and inducers of CYPs and transporters, the Knowledgebase provides useful information on the compounds therapeutic class, clinical recommended dosage, pharmacokinetics (e.g., dose proportionality accumulation ratio, time to steady-state), QT prolongation, and NTI characteristics.

As always, feel free to contact us if you have any questions or comments.

In September, we added 83 citations in DIDB, including 44 in vitro (with 24 articles published in September 2024) and 39 in vivo articles (with 27 articles published in September 2024).

6 NDA/BLAs approved in 2024, including axatilimab (NIKTIMVO), deuroxolitinib (LEQSELVI), lazertinib (LAZCLUZE), nemolizumab (NEMLUVIO), palopegteriparatide (YORVIPATH), and vorasidenib (VORANIGO), were also curated in DIDB.

You can check the citations that are recently published and entered in DIDB and all the NDAs/BLAs in DIDB.

As always, feel free to contact us if you have any questions or comments.

In August, we added 115 citations in DIDB, including 47 in vitro (with 28 articles published in August 2024) and 68 in vivo articles (with 38 articles published in August 2024).

2 NDA/BLAs approved in 2024, including elafibranor (IQIRVO) and donanemab (KISUNLA), were also curated in DIDB.

You can check the citations that are recently published and entered in DIDB and all the NDAs/BLAs in DIDB.

As always, feel free to contact us if you have any questions or comments.

In July, we added 127 citations in DIDB, including 70 in vitro (with 17 articles published in July 2024) and 57 in vivo articles (with 41 articles published in July 2024).

4 NDA/BLAs approved in 2024, including crovalimab (PIASKY), imetelstat (RYTELO), sofpironium (SOFDRA), and tarlatamab (IMDELLTRA), were also curated in DIDB.

You can check the citations that are recently published and entered in DIDB and all the NDAs/BLAs in DIDB.

As always, feel free to contact us if you have any questions or comments.

To enhance accessibility to PBPK data, a “PBPK Study” tag has been introduced at the citation level. This tag will appear alongside the citation/NDA number for any citation/NDA containing PBPK data. An example is provided below:

With this new feature, you can now easily identify citations and NDA/BLAs that include PBPK data in the tables of citations or NDA/BLAs recently published in DIDB. Simply use “PBPK” as a filter in the Accession # and NDA/BLA # columns to find relevant entries. You can use the following searches: citations that are recently published and entered in DIDB and all the NDAs/BLAs in DIDB to try this new feature.

As always, feel free to contact us if you have any questions or comments.

In June, we added 93 citations in DIDB, including 48 in vitro (with 16 articles published in June 2024) and 45 in vivo articles (with 41 articles published in June 2024).

3 NDAs approved in 2024, including ceftobiprole (ZEVTERA), danicopan (VOYDEYA), and mavorixafor (XOLREMDI), were also curated in DIDB.

You can check the citations that are recently published and entered in DIDB and all the NDAs/BLAs in DIDB.

As always, feel free to contact us if you have any questions or comments.

The DDI Marker Studies Knowledgebase has been updated in July 2024 and is available in the DIDB Resource Center.

Our Editorial Team has dedicated effort on identifying substrates and inhibitors for OAT1, OAT3, OCT2, MATE1, and MATE2-K transporters. In this update, we have added 29 substrates and inhibitors of these transporters. Overall, 60 compounds have been identified as substates, inhibitors, and inducers of CYP enzymes and various transporters, including P-gp, BCRP, OATP1B1, OATP1B3, OAT1, OAT3, OCT2, MATE1, and MATE2-K. Notably, two compounds are classified as sensitive substrates of CYP3A, and a compound previously considered a moderate CYP2D6 inhibitor is now recognized as a strong inhibitor based on recent DDI data. These compounds could potentially lead to significant drug interactions mediated by these CYPs.

To view a comprehensive list of additions and modifications, including new compounds and updates to existing entries, you may use the “Recent Update” column (Column AE) on the spreadsheet and select “yes.”

In addition to substrates, inhibitors and inducers of CYPs and transporters, the Knowledgebase provides useful information on the compounds therapeutic class, clinical recommended dosage, pharmacokinetics (e.g., dose proportionality accumulation ratio, time to steady-state), QT prolongation, and NTI characteristics.

As always, feel free to contact us if you have any questions or comments.