Literature DB >> 19550005

Some considerations concerning volume-modulated arc therapy: a stepping stone towards a general theory.

S Webb1, D McQuaid.   

Abstract

In this paper it is formally shown that the dynamic multileaf collimator (MLC) IMRT delivery technique remains valid if the MLC is supported on a 1D moving platform. It is also shown that, in such circumstances, it is always time preferable to deliver overlapping modulating fields as a single swept field rather than as separate fields. The most general formulism is presented and then related to simpler equations in limiting cases. The paper explains in detail how a 'small-arc approximation' can be invoked to relate the 1D linear theory to the MLC-on-moving-platform-(gantry) delivery technique involving rotation therapy and known as volume-modulated arc therapy (VMAT). It is explained how volume-modulated arc therapy delivered with open unmodulated fields and which can deliver conformal dose distributions can be interpreted as an IMRT delivery. The (Elekta adopted) term VMAT will be used in a generic sense to include a similar (Varian) method known as RapidArc. Approximate expressions are derived for the 'amount of modulation' possible in a VMAT delivery. This paper does not discuss the actual VMAT planning but gives an insight at a deep level into VMAT delivery. No universal theory of VMAT is known in the sense that there is no theory that can predict precisely the performance of a VMAT delivery in terms of the free parameters available (variable gantry speed, variable fluence-delivery rate, set of MLC shapes, MLC orientation, number of arcs, coplanarity versus non-coplanarity, etc). This is in stark contrast to the situation with several other IMRT delivery techniques where such theoretical analyses are known. In this paper we do not provide such a theory; the material presented is a stepping stone on the path towards this.

Mesh:

Year:  2009        PMID: 19550005     DOI: 10.1088/0031-9155/54/14/001

Source DB:  PubMed          Journal:  Phys Med Biol        ISSN: 0031-9155            Impact factor:   3.609


  13 in total

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Journal:  J Med Phys       Date:  2016 Jul-Sep
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