Synthesis of 11,12-dihydro benzo[c]phenanthridines via a Pd-catalyzed unusual construction of isocoumarin ring/FeCl3-mediated intramolecular arene-allyl cyclization: First identification of a benzo[c]phenanthridine based PDE4 inhibitor

B. Thirupataiah; Gangireddy Sujeevan Reddy; Shailendra S. Ghule; Jetta Sandeep Kumar; Guntipally Mounika; Kazi Amirul Hossain; Jayesh Mudgal; Jessy E. Mathew; Gautham G. Shenoy; Kishore V.L. Parsa; Manojit Pal

doi:10.1016/j.bioorg.2020.103691

Synthesis of 11,12-dihydro benzo[c]phenanthridines via a Pd-catalyzed unusual construction of isocoumarin ring/FeCl₃-mediated intramolecular arene-allyl cyclization: First identification of a benzo[c]phenanthridine based PDE4 inhibitor

B. Thirupataiah, Gangireddy Sujeevan Reddy, Shailendra S. Ghule, Jetta Sandeep Kumar, Guntipally Mounika, Kazi Amirul Hossain, Jayesh Mudgal, Jessy E. Mathew, Gautham G. Shenoy, Kishore V.L. Parsa, Manojit Pal

Department of Pharmacology, Manipal College of Pharmaceutical Sciences, Manipal
Department of Pharmaceutical Chemistry, Manipal College of Pharmaceutical Sciences, Manipal

Research output: Contribution to journal › Article › peer-review

7 Citations (Scopus)

Abstract

In spite of their various pharmacological properties the anti-inflammatory potential of benzo[c]phenanthridines remained underexplored. Thus, for the first time PDE4 inhibitory potential of 11,12-dihydro benzo[c]phenanthridine/benzo[c]phenanthridine was assessed in vitro. Elegant synthesis of these compounds was performed via a multi-step sequence consisting of a Pd-catalyzed unusual construction of 4-allyl isocoumarin ring and FeCl₃-mediated intramolecular regio- as well as site-selective arene-allyl cyclization as key steps. The overall strategy involved Sonogashira coupling followed by isocoumarin and isoquinolone synthesis, then chlorination and subsequent cyclization to afford a range of 11,12-dihydro derivatives. One of these dihydro compounds was converted to the corresponding benzo[c]phenanthridine that showed concentration dependent inhibition of PDE4B affording an initial hit molecule. The SAR study suggested that 11,12-dihydro analogs were less potent than the compound having unsaturation at the same part of the ring.

Original language	English
Article number	103691
Journal	Bioorganic Chemistry
Volume	97
DOIs	https://doi.org/10.1016/j.bioorg.2020.103691
Publication status	Published - 04-2020

All Science Journal Classification (ASJC) codes

Biochemistry
Molecular Biology
Drug Discovery
Organic Chemistry

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Thirupataiah, B., Reddy, G. S., Ghule, S. S., Kumar, J. S., Mounika, G., Hossain, K. A., Mudgal, J., Mathew, J. E., Shenoy, G. G., Parsa, K. V. L., & Pal, M. (2020). Synthesis of 11,12-dihydro benzo[c]phenanthridines via a Pd-catalyzed unusual construction of isocoumarin ring/FeCl₃-mediated intramolecular arene-allyl cyclization: First identification of a benzo[c]phenanthridine based PDE4 inhibitor. Bioorganic Chemistry, 97, [103691]. https://doi.org/10.1016/j.bioorg.2020.103691

@article{d0cb4d1180254b3faef3976d6ca186f4,

title = "Synthesis of 11,12-dihydro benzo[c]phenanthridines via a Pd-catalyzed unusual construction of isocoumarin ring/FeCl3-mediated intramolecular arene-allyl cyclization: First identification of a benzo[c]phenanthridine based PDE4 inhibitor",

abstract = "In spite of their various pharmacological properties the anti-inflammatory potential of benzo[c]phenanthridines remained underexplored. Thus, for the first time PDE4 inhibitory potential of 11,12-dihydro benzo[c]phenanthridine/benzo[c]phenanthridine was assessed in vitro. Elegant synthesis of these compounds was performed via a multi-step sequence consisting of a Pd-catalyzed unusual construction of 4-allyl isocoumarin ring and FeCl3-mediated intramolecular regio- as well as site-selective arene-allyl cyclization as key steps. The overall strategy involved Sonogashira coupling followed by isocoumarin and isoquinolone synthesis, then chlorination and subsequent cyclization to afford a range of 11,12-dihydro derivatives. One of these dihydro compounds was converted to the corresponding benzo[c]phenanthridine that showed concentration dependent inhibition of PDE4B affording an initial hit molecule. The SAR study suggested that 11,12-dihydro analogs were less potent than the compound having unsaturation at the same part of the ring.",

author = "B. Thirupataiah and Reddy, {Gangireddy Sujeevan} and Ghule, {Shailendra S.} and Kumar, {Jetta Sandeep} and Guntipally Mounika and Hossain, {Kazi Amirul} and Jayesh Mudgal and Mathew, {Jessy E.} and Shenoy, {Gautham G.} and Parsa, {Kishore V.L.} and Manojit Pal",

year = "2020",

month = apr,

doi = "10.1016/j.bioorg.2020.103691",

language = "English",

volume = "97",

journal = "Bioorganic Chemistry",

issn = "0045-2068",

publisher = "Academic Press Inc.",

}

Thirupataiah, B, Reddy, GS, Ghule, SS, Kumar, JS, Mounika, G, Hossain, KA, Mudgal, J , Mathew, JE , Shenoy, GG, Parsa, KVL & Pal, M 2020, 'Synthesis of 11,12-dihydro benzo[c]phenanthridines via a Pd-catalyzed unusual construction of isocoumarin ring/FeCl₃-mediated intramolecular arene-allyl cyclization: First identification of a benzo[c]phenanthridine based PDE4 inhibitor', Bioorganic Chemistry, vol. 97, 103691. https://doi.org/10.1016/j.bioorg.2020.103691

Synthesis of 11,12-dihydro benzo[c]phenanthridines via a Pd-catalyzed unusual construction of isocoumarin ring/FeCl₃-mediated intramolecular arene-allyl cyclization: First identification of a benzo[c]phenanthridine based PDE4 inhibitor. / Thirupataiah, B.; Reddy, Gangireddy Sujeevan; Ghule, Shailendra S. et al.
In: Bioorganic Chemistry, Vol. 97, 103691, 04.2020.

Research output: Contribution to journal › Article › peer-review

TY - JOUR

T1 - Synthesis of 11,12-dihydro benzo[c]phenanthridines via a Pd-catalyzed unusual construction of isocoumarin ring/FeCl3-mediated intramolecular arene-allyl cyclization

T2 - First identification of a benzo[c]phenanthridine based PDE4 inhibitor

AU - Thirupataiah, B.

AU - Reddy, Gangireddy Sujeevan

AU - Ghule, Shailendra S.

AU - Kumar, Jetta Sandeep

AU - Mounika, Guntipally

AU - Hossain, Kazi Amirul

AU - Mudgal, Jayesh

AU - Mathew, Jessy E.

AU - Shenoy, Gautham G.

AU - Parsa, Kishore V.L.

AU - Pal, Manojit

PY - 2020/4

Y1 - 2020/4

N2 - In spite of their various pharmacological properties the anti-inflammatory potential of benzo[c]phenanthridines remained underexplored. Thus, for the first time PDE4 inhibitory potential of 11,12-dihydro benzo[c]phenanthridine/benzo[c]phenanthridine was assessed in vitro. Elegant synthesis of these compounds was performed via a multi-step sequence consisting of a Pd-catalyzed unusual construction of 4-allyl isocoumarin ring and FeCl3-mediated intramolecular regio- as well as site-selective arene-allyl cyclization as key steps. The overall strategy involved Sonogashira coupling followed by isocoumarin and isoquinolone synthesis, then chlorination and subsequent cyclization to afford a range of 11,12-dihydro derivatives. One of these dihydro compounds was converted to the corresponding benzo[c]phenanthridine that showed concentration dependent inhibition of PDE4B affording an initial hit molecule. The SAR study suggested that 11,12-dihydro analogs were less potent than the compound having unsaturation at the same part of the ring.

AB - In spite of their various pharmacological properties the anti-inflammatory potential of benzo[c]phenanthridines remained underexplored. Thus, for the first time PDE4 inhibitory potential of 11,12-dihydro benzo[c]phenanthridine/benzo[c]phenanthridine was assessed in vitro. Elegant synthesis of these compounds was performed via a multi-step sequence consisting of a Pd-catalyzed unusual construction of 4-allyl isocoumarin ring and FeCl3-mediated intramolecular regio- as well as site-selective arene-allyl cyclization as key steps. The overall strategy involved Sonogashira coupling followed by isocoumarin and isoquinolone synthesis, then chlorination and subsequent cyclization to afford a range of 11,12-dihydro derivatives. One of these dihydro compounds was converted to the corresponding benzo[c]phenanthridine that showed concentration dependent inhibition of PDE4B affording an initial hit molecule. The SAR study suggested that 11,12-dihydro analogs were less potent than the compound having unsaturation at the same part of the ring.

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U2 - 10.1016/j.bioorg.2020.103691

DO - 10.1016/j.bioorg.2020.103691

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JO - Bioorganic Chemistry

JF - Bioorganic Chemistry

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Thirupataiah B, Reddy GS, Ghule SS, Kumar JS, Mounika G, Hossain KA et al. Synthesis of 11,12-dihydro benzo[c]phenanthridines via a Pd-catalyzed unusual construction of isocoumarin ring/FeCl₃-mediated intramolecular arene-allyl cyclization: First identification of a benzo[c]phenanthridine based PDE4 inhibitor. Bioorganic Chemistry. 2020 Apr;97:103691. doi: 10.1016/j.bioorg.2020.103691