Hydrogen-bridged bis(silylene) complexes of ruthenium and iron: synthesis, structures and multi-centre bonding interactions at the M–Si–H–Si four-membered ring

The molecule of the title compound, C15H26Cl2, is built up from two fused six-membered and seven-membered rings. The six-membered ring has a perfect chair conformation, whereas the seven-membered ring displays a twist-chair conformation. A weak C—H...Cl hydrogen-bonding interaction links the molecule into a chain parallel to the a axis.

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Carbocyclic Three- and Four-Membered Ring Compounds

10.1055/b-003-109677 ◽

1997 ◽

Keyword(s):

Membered Ring ◽

Ring Compounds

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Mechanical Stability and Self-Recovery Property of Liquid Crystal Gel Films with Hydrogen-Bonding Interaction

IEICE Transactions on Electronics ◽

10.1587/transele.2019dis0003 ◽

2019 ◽

Vol E102.C (11) ◽

pp. 813-817

Author(s):

Yosei SHIBATA ◽

Ryosuke SAITO ◽

Takahiro ISHINABE ◽

Hideo FUJIKAKE

Keyword(s):

Hydrogen Bonding ◽

Liquid Crystal ◽

Mechanical Stability ◽

Hydrogen Bonding Interaction ◽

Bonding Interaction

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An Alternate Energy-Conserved Pathway for the Morita-Baylis-Hillman (MBH) Reaction

10.26434/chemrxiv.12011673.v1 ◽

2020 ◽

Author(s):

Veejendra Yadav

Keyword(s):

Proton Transfer ◽

Transition State ◽

Lower Energy ◽

Aldol Reaction ◽

Membered Ring ◽

Ammonium Ion ◽

Alternate Energy ◽

Ring Transition State ◽

Mbh Reaction

An new overall lower energy pathway for the amine-catalysed Morita-Baylis-Hillman reaction is proposed from computations at the M06-2X/6-311++G(d,p) level. The pathway involves proton-transfer from the ammonium ion to the alkoxide formed from the aldol reaction through a seven-membered ring transition state (TS) structure followed by highly exothermic Hofmann<i> </i>elimination through a five-membered ring TS structure to form the product and also release the catalyst to carry on with the process all over again.

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An Alternate Energy-Conserved Pathway for the Morita-Baylis-Hillman (MBH) Reaction

10.26434/chemrxiv.12011673 ◽

2020 ◽

Author(s):

Veejendra Yadav

Keyword(s):

Proton Transfer ◽

Transition State ◽

Lower Energy ◽

Aldol Reaction ◽

Membered Ring ◽

Ammonium Ion ◽

Alternate Energy ◽

Ring Transition State ◽

Mbh Reaction

An new overall lower energy pathway for the amine-catalysed Morita-Baylis-Hillman reaction is proposed from computations at the M06-2X/6-311++G(d,p) level. The pathway involves proton-transfer from the ammonium ion to the alkoxide formed from the aldol reaction through a seven-membered ring transition state (TS) structure followed by highly exothermic Hofmann<i> </i>elimination through a five-membered ring TS structure to form the product and also release the catalyst to carry on with the process all over again.

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Radical Enzymes Control the Chemistry of Their Highly Reactive Intermediates Using the Quantum Coulombic Effect

10.26434/chemrxiv.12839177.v1 ◽

2020 ◽

Author(s):

Hossein Khalilian ◽

Gino A. DiLabio

Keyword(s):

Hydrogen Bonding ◽

Molecular Orbital ◽

Reactive Intermediates ◽

Hydrogen Bonding Interaction ◽

Orbital Ordering ◽

Dynamic Nature ◽

Radical Intermediate ◽

Highest Occupied Molecular Orbital ◽

Bonding Interaction ◽

Close Proximity

Here, we report an exquisite strategy that the B12 enzymes exploit to manipulate the reactivity of their radical intermediate (Adenosyl radical). Based on the quantum-mechanic calculations, these enzymes utilize a little known long-ranged through space quantum Coulombic effect (QCE). The QCE causes the radical to acquire an electronic structure that contradicts the Aufbau Principle: The singly-occupied molecular orbital (SOMO) is no longer the highest-occupied molecular orbital (HOMO) and the radical is unable to react with neighbouring substrates. The dynamic nature of the enzyme and its structure is expected to be such that the reactivity of the radical is not restored until it is moved into close proximity of the target substrate. We found that the hydrogen bonding interaction between the nearby conserved glutamate residue and the ribose ring of Adenosyl radical plays a crucial role in manipulating the orbital ordering

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Radical Enzymes Control the Chemistry of Their Highly Reactive Intermediates Using the Quantum Coulombic Effect

10.26434/chemrxiv.12839177 ◽

2020 ◽

Author(s):

Hossein Khalilian ◽

Gino A. DiLabio

Keyword(s):

Hydrogen Bonding ◽

Molecular Orbital ◽

Reactive Intermediates ◽

Hydrogen Bonding Interaction ◽

Orbital Ordering ◽

Dynamic Nature ◽

Radical Intermediate ◽

Highest Occupied Molecular Orbital ◽

Bonding Interaction ◽

Close Proximity

Here, we report an exquisite strategy that the B12 enzymes exploit to manipulate the reactivity of their radical intermediate (Adenosyl radical). Based on the quantum-mechanic calculations, these enzymes utilize a little known long-ranged through space quantum Coulombic effect (QCE). The QCE causes the radical to acquire an electronic structure that contradicts the Aufbau Principle: The singly-occupied molecular orbital (SOMO) is no longer the highest-occupied molecular orbital (HOMO) and the radical is unable to react with neighbouring substrates. The dynamic nature of the enzyme and its structure is expected to be such that the reactivity of the radical is not restored until it is moved into close proximity of the target substrate. We found that the hydrogen bonding interaction between the nearby conserved glutamate residue and the ribose ring of Adenosyl radical plays a crucial role in manipulating the orbital ordering

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Catalytic Synthesis of Cyclic Guanidines via Hydrogen Atom Transfer and Radical-Polar Crossover

10.26434/chemrxiv.13318421.v1 ◽

2020 ◽

Author(s):

Shunya Ohuchi ◽

Hiroki Koyama ◽

Hiroki Shigehisa

Keyword(s):

Hydrogen Atom ◽

Functional Group ◽

Hydrogen Atom Transfer ◽

Catalytic Synthesis ◽

Membered Ring ◽

Biologically Active ◽

Atom Transfer ◽

Powerful Method ◽

Protective Groups ◽

The Common

A catalytic synthesis of cyclic guanidines, which are found in many biologically active compounds and natu-ral products, was developed, wherein transition-metal hydrogen atom transfer and radical-polar crossover were employed. This mild and functional-group tolerant process enabled the cyclization of alkenyl guanidines bearing common protective groups, such as Cbz and Boc. This powerful method not only provided the common 5- and 6-membered rings but also an unusual 7-membered ring. The derivatization of the products afforded various heterocycles. We also investigated the se-lective cyclization of mono-protected or hetero-protected (TFA and Boc) alkenyl guanidines and their further derivatiza-tions.

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Convergent Total Synthesis of Principinol D, a Rearranged Kaurane Diterpenoid

10.26434/chemrxiv.7865168.v4 ◽

2019 ◽

Author(s):

Timothy Newhouse ◽

Aneta Turlik ◽

Yifeng Chen ◽

Anthony Scruse

Keyword(s):

Total Synthesis ◽

Natural Product ◽

Late Stage ◽

Membered Ring ◽

Entry Point ◽

Ketone Reduction ◽

Coupling Approach

<div> <p>The total synthesis of principinol D, a rearranged kaurane diterpenoid, is reported. This grayanane natural product is constructed via a convergent fragment coupling approach, wherein the central 7-membered ring is synthesized at a late stage. The bicyclo[3.2.1]octane fragment is accessed by a Ni-catalyzed α-vinylation reaction. Strategic reductions include a diastereoselective SmI<sub>2</sub>-mediated ketone reduction with PhSH and a new protocol for selective ester reduction in the presence of ketones. The convergent strategy reported herein may be an entry point to the larger class of kaurane diterpenoids.</p> </div>

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